SECURITIES AND EXCHANGE COMMISSION
Washington, D.C. 20549
☒ ANNUAL REPORT PURSUANT TO SECTION
13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934
For the fiscal year ended: December 31,
☐ TRANSITION REPORT PURSUANT TO SECTION
13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934
For the transition period from _____________
Commission File No. 000-52545
Wize Pharma, Inc.
(Exact name of registrant as specified in
(State or other jurisdiction of
incorporation or organization)
5b Hanagar Street, Hod Hasharon, Israel,
(Address of principal executive offices)
Issuer’s telephone number: +972
Securities Registered pursuant to Section
12(b) of the Act: None
Securities Registered pursuant to Section
12(g) of the Exchange Act: Common Stock, $0.001 Par Value
Indicate by check mark if the registrant is a well-known seasoned
issuer, as defined in Rule 405 of the Securities Act.
Yes ☐ No ☒
Indicate by check mark if the registrant is not required to
file reports pursuant to Section 13 or 15(d) of the Act.
Yes ☐ No ☒
Indicate by check mark whether the registrant
(1) has filed all reports required to be filed by section 13 or 15(d) of the Securities Exchange Act of 1934 during the preceding
12 months (or for such shorter period that the registrant was required to file such reports), and (2) has been subject to such
filing requirements for the past 90 days.
Yes ☒ No ☐
Indicate by check mark whether the registrant
has submitted electronically and posted on its corporate Website, if any, every Interactive Data File required to be submitted
and posted pursuant to Rule 405 of Regulation S-T (§232.405 of this chapter) during the preceding 12 months (or for such shorter
period that the registrant was required to submit and post such files).
Yes ☒ No ☐
Indicate by check mark if disclosure of
delinquent filers pursuant to Item 405 of Regulation S-K (§229.405 of this chapter) is not contained herein, and will not
be contained, to the best of registrant’s knowledge, in definitive proxy or information statements incorporated by reference
in Part III of this Form 10-K or any amendment to this Form 10-K. ☐
Indicate by check mark whether the registrant
is a large accelerated filer, an accelerated filer, a non-accelerated filer, or a smaller reporting company. See the definitions
of “large accelerated filer,” “accelerated filer”, “smaller reporting company,” and “emerging
growth company” in Rule 12b-2 of the Exchange Act.
|Large accelerated filer: ☐
||Accelerated filer: ☐|
|Non-accelerated filer: ☐
||Smaller reporting company: ☒|
|(Do not check if a smaller reporting company)
||Emerging growth company: ☒|
If an emerging growth company, indicate
by check mark if the registrant has elected not to use the extended transition period for complying with any new or revised financial
accounting standards provided pursuant to Section 13(a) of the Exchange Act ☒
Indicate by check mark whether the registrant is a shell company
(as defined in Rule 12b-2 of the Act).
Yes ☐ No ☒
The aggregate market value of the voting
and non-voting common equity held by non-affiliates of the registrant was $945,458 computed by reference to the average bid and
asked price of the Common Stock as of the last business day of the registrant’s most recently completed second fiscal quarter.
As of March 28, 2018, there were 4,925,742
shares of the registrant’s Common Stock outstanding.
DOCUMENTS INCORPORATED BY REFERENCE:
TABLE OF CONTENTS
CAUTIONARY STATEMENT REGARDING FORWARD-LOOKING
This Annual Report on Form 10-K (this
“Annual Report”) (including the section regarding Management’s Discussion and Analysis of Financial Condition
and Results of Operations) contains forward-looking statements, about our expectations, beliefs or intentions regarding, among
other things, our product development efforts, business, financial condition, results of operations, strategies or prospects. In
addition, from time to time, our representatives have made or may make forward-looking statements, orally or in writing. Forward-looking
statements can be identified by the use of forward-looking words such as “believe,” “expect,” “intend,”
“plan,” “may,” “should” or “anticipate” or their negatives or other variations
of these words or other comparable words or by the fact that these statements do not relate strictly to historical or current matters.
These forward-looking statements may be included in, but are not limited to, various filings made by us with the United States
Securities and Exchange Commission, or the SEC, press releases or oral statements made by or with the approval of one of our authorized
executive officers. Forward-looking statements relate to anticipated or expected events, activities, trends or results as of the
date they are made. Because forward-looking statements relate to matters that have not yet occurred, these statements are inherently
subject to risks and uncertainties that could cause our actual results to differ materially from any future results expressed or
implied by the forward-looking statements. Many factors could cause our actual activities or results to differ materially from
the activities and results anticipated in forward-looking statements, including, but not limited to, the factors summarized below.
Report identifies important factors which could cause our actual results to differ materially from those indicated by the
forward-looking statements, particularly those set forth under Item 1A - “RISK FACTORS,” beginning on page 35 of
this Annual Report. The risk factors included in this Annual Report are not necessarily all of the important factors that
could cause actual results to differ materially from those expressed in any of our forward-looking statements. Given these
uncertainties, you are cautioned not to place undue reliance on such forward-looking statements. Factors that could cause our
actual results to differ materially from those expressed or implied in such forward-looking statements include, but are not
||we have substantial debt which may adversely affect us by limiting future sources of financing, interfering with our ability to pay interest and principal on our indebtedness and subjecting us to additional risks;|
||we need to raise additional capital to meet our business requirements in the future, and such capital raising may be costly or difficult to obtain and will dilute current stockholders’ ownership interests;|
||our current pipeline is based on a single compound known as LO2A (“LO2A”) and on the continuation of our license to commercialize LO2A;|
||our inability to expand our rights under our license agreement for LO2A may have a detrimental effect on our business;|
||the initiation, timing, progress and results of our preclinical studies, clinical trials and other product candidate development efforts;|
||our ability to advance our product candidate into clinical trials or to successfully complete our preclinical studies or clinical trials;|
||our receipt of regulatory approvals for our product candidate, and the timing of other regulatory filings and approvals;|
||the clinical development, commercialization and market acceptance of LO2A;|
||our ability to establish and maintain corporate collaborations;|
||the implementation of our business model and strategic plans for its business and product candidate;|
||the scope of protection we are able to establish and maintain for intellectual property rights covering LO2A and its ability to operate its business without infringing the intellectual property rights of others;|
||estimates of our expenses, future revenues, and capital requirements;|
||competitive companies, technologies and its industry; and|
||statements as to the impact of the political and security situation in Israel on our business.|
statements attributable to us or persons acting on our behalf speak only as of the date of this Annual Report and are expressly
qualified in their entirety by the cautionary statements included in this Annual Report. We undertake no obligations to update
or revise forward-looking statements to reflect events or circumstances that arise after the date made or to reflect the occurrence
of unanticipated events. In evaluating forward-looking statements, you should consider these risks and uncertainties.
Throughout this Annual Report, unless
otherwise designated, the terms “we,” “us,” “our,” the “Company,” “Wize”
and “our company” refer to Wize Pharma, Inc. (formerly known as OphthaliX, Inc.), a Delaware corporation, and its
wholly-owned Israeli subsidiary, Wize Pharma Ltd. (“Wize Israel”).
All dollar amounts refer to U.S. dollars
unless otherwise indicated.
Unless derived from Wize’s financial
statements or otherwise indicated, U.S. dollar translations of New Israeli Shekels (“NIS”) amounts presented in this
report are translated using the rate of NIS 3.495 to one U.S. dollar, the exchange rate reported by the Bank of Israel for
March 21, 2018.
On March 5, 2018, we effected a reverse
stock split of our Common Stock at a ratio of one for twenty-four (1:24), or the Reverse Stock Split. Unless otherwise indicated,
all share and per share amounts included in this Annual Report have been adjusted retroactively to reflect the effects of the Reverse
Wize Pharma, Inc.®, the
Wize logo and other trademarks or service marks of Wize appearing in this Annual Report are the property of Wize or its subsidiaries.
Trade names, trademarks and service marks of other companies appearing in this Annual Report are the property of their respective
ITEM 1. BUSINESS.
We are a clinical-stage biopharmaceutical
company currently focused on the treatment of ophthalmic disorders, including dry eye syndrome (“DES”). We have in-licensed
certain rights to purchase, market, sell and distribute a formula known as LO2A, a drug developed for the treatment of DES,
and other ophthalmological illnesses, including Conjunctivochalasis (“CCH”) and Sjögren’s syndrome (“Sjögren’s”).
LO2A is currently registered and marketed
by its inventor in Germany and Switzerland for the treatment of DES, in Hungary for the treatment of DES and CCH and in the Netherlands
for the treatment of DES and Sjögren’s.
We intend to market LO2A as a treatment
for DES and other ophthalmic inflammations, including CCH and Sjögren’s in the United States, Israel, Ukraine and the
People’s Republic of China (“China”), subject to certain conditions (collectively, the “Licensed Territories”),
the territories that we have licensed LO2A, and in additional territories, subject to purchasing the rights to market, sell and
distribute LO2A in those additional territories. We believe that the potential for the most economic success is in marketing LO2A
for treating CCH and Sjögren’s. Currently, we have a distribution agreement for marketing in Israel, where LO2A is approved
for the treatment of DES only, a distribution agreement for marketing in Ukraine, where LO2A is in the approval process for the
treatment of DES and CCH, and a framework agreement for distribution in China, where the preparation for the registration process
commenced in December 2017 by the Chinese Distributor (as defined below). The registration process in certain countries, including
the United States, requires us to conduct additional clinical trials, in addition to the Phase II clinical trial that we are currently
We plan to engage local or multinational
distributors to handle the distribution of LO2A. In particular, we intend to engage, subject to obtaining the requisite rights
in LO2A, pharmaceutical companies or distributors around the world with relevant marketing capabilities in the pharmaceutical
field, in order for such pharmaceutical companies to sell LO2A, with us prioritizing those territories where we may expedite the
registration process of LO2A based on existing knowledge and studies previously conducted on LO2A, without requiring additional
In February 2018, we received Institutional
Review Board (IRB) approval for the protocol of our planned Phase IV study, which is a randomized, double-masked, study of LO2A
versus Alcon’s Systane® Ultra UD, an over-the-counter lubricant eye drop product used to relieve dry and
irritated eyes (the “Phase IV Study”). The Phase IV Study will take place in Israel and will evaluate the safety and
efficacy of LO2A for symptomatic improvement of DES in 60 adult patients with Sjögren’s. Enrolled patients will be
randomized in a 1:1 ratio to one of two treatment groups, LO2A or Systane® Ultra UD. Drops will be administered
topically to the eye over a three month period. This Phase IV Study is designed to support our clinical approval pathway for LO2A
for the treatment of DES in patients with Sjögren’s within certain markets including the U.S., China, Ukraine and Israel.
We enrolled our first patient in the Phase IV Study in the end of March 2018. We currently do not have sufficient funds to complete
the Phase IV Study. The completion of such study is contingent upon our ability to raise additional funds.
Historical Background and Corporate Details
We were originally incorporated in the State
of Nevada on December 10, 1999, under the name Bridge Capital.com, Inc., which was a nominally capitalized corporation that did
not commence its operations until it changed its name to Denali Concrete Management, Inc., or Denali, in March 2001. Denali was
a concrete placement company specializing in providing concrete improvements in the road construction industry and operated primarily
in Anchorage, Alaska, placing curb and gutter, sidewalks and retaining walls for state, municipal and military projects. In December
2005, Denali ceased its principal business operations and focused its efforts on seeking a business opportunity.
Denali consummated a reverse merger transaction
on November 21, 2011, in connection with which the following events occurred:
||We entered into and completed a stock purchase agreement with Can-Fite BioPharma Ltd. (“Can-Fite”), our former controlling shareholder, whereby Can-Fite purchased 333,333 of shares of our common stock, $0.001 par value (“Common Stock”) in exchange for all of the issued and outstanding ordinary shares of Eye-Fite Ltd. (“Eye-Fite”). As a result of the consummation of the actions contemplated by such agreement, Eyefite became our wholly-owned subsidiary and Can-Fite became our majority stockholder and a parent;|
||Eyefite and Can-Fite entered into a license agreement dated November 21, 2011 (the “Can-Fite License Agreement”) pursuant to which Can-Fite granted to Eyefite a sole and exclusive worldwide license for the use of CF101, Can-Fite’s therapeutic drug candidate, solely in the field of ophthalmic indications; and|
||Eyefite and Can-Fite entered into a services agreement dated November 21, 2011 (the “Eyefite Services Agreement”) pursuant to which Can-Fite managed, as an independent contractor, all activities relating to pre-clinical and clinical studies performed for the development of the ophthalmic indications of CF101.|
Upon completion of the reverse merger, and
after giving effect to the transactions described above, we had an aggregate of 435,052 issued and outstanding shares of Common
Stock. Of these shares, Can-Fite owned approximately 82%. Following the transactions, we, through our wholly owned subsidiary,
Eyefite, became a clinical-stage biopharmaceutical company focused on developing therapeutic products for the treatment of ophthalmic
On January 25, 2012, we changed our name
and trading symbol on the OTC Pink to OphthaliX Inc. and OPLI, respectively. On February 6, 2012, our majority stockholder, Can-Fite,
approved (a) a change in our state of incorporation from the State of Nevada to the State of Delaware and (b) an amendment to our
Certificate of Incorporation to increase the number of authorized shares of Common Stock, from
50,000,000 to 100,000,000. The effective date for these changes was April 2, 2012.
On July 18, 2013, our stockholders approved
a reverse stock split of one share of our Common Stock for each four and one-half shares outstanding (1:4.5). The reverse split
became effective as of the close of business on August 6, 2013.
On September 21, 2016, after a unanimous
vote by our Board of Directors, or Board, on September 19, 2016, our majority stockholder, Can-Fite, approved (1) our voluntary
dissolution and liquidation pursuant to a Plan of Dissolution, and (2) the re-election of the following five directors, to comprise
the entire board of directors, to serve until the next annual meeting of stockholders and until their successors are elected and
qualified: Pnina Fishman, Ilan Cohn, Guy Regev, Roger Kornfeld and Michael Belkin. The Plan of Dissolution was expected to go into
effect 20 days after the date an information statement (the “Definitive Information Statement”) was first given to
all our stockholders who did not execute the written consent of Can-Fite.
Prior to the distribution of the Definitive
Information Statement, on November 10, 2016, our Board of Directors abandoned its voluntary dissolution and liquidation. On the
same day, our Board of Directors authorized its entry into a non-binding letter of intent with Wize Israel for a proposed reverse
merger. Subsequently, on May 21, 2017, we entered into an Agreement and Plan of Merger (as amended, the “Merger Agreement”),
with Bufiduck Ltd., a company formed under the laws of the State of Israel and our wholly owned subsidiary (“Merger Sub”)
and Wize Israel, which contemplated the merger of Merger Sub with and into Wize Israel, with Wize Israel continuing as the surviving
entity and becoming our wholly owned subsidiary (the “Merger”). The dissolution mentioned above was suspended following
our agreement with Wize Israel to effect the Merger pursuant to the Merger Agreement and the re-election of directors was not effected.
On October 10, 2017, at our annual meeting
of stockholders (the “2017 Annual Meeting”), our stockholders approved, among other matters, (a) an amendment to our
Certificate of Incorporation to increase the number of authorized shares of Common Stock, from
100,000,000 to 500,000,000, (b) an amendment to our Certificate of Incorporation to change our name from “OphthaliX, Inc.”
to “Wize Pharma, Inc.” immediately prior to the Merger, and (c) the re-election of Pnina Fishman, Ilan Cohn, Guy Regev,
Roger Kornberg and Michael Belkin to hold office until the next annual meeting of stockholders and until their respective successors
are duly elected and qualified; provided, however, that, if the Merger is completed, our Board of Directors will be reconstituted
as described in the proxy statement/prospectus relating to our 2017 Annual Meeting.
On October 31, 2017, Merger Sub, Wize Israel
and us entered into an amendment to the Merger Agreement which extended the expiration date of the Merger Agreement until November
On November 16,
2017 (the “Closing Date”), we were renamed “Wize Pharma, Inc.,” and completed our transaction with Wize
Israel in accordance with the terms of the Merger Agreement pursuant to which Merger Sub merged with and into Wize Israel, with
Wize Israel surviving as our wholly owned subsidiary. Prior to the Merger, we had no active business and were a “shell company”
as such term is defined in Rule 12b-2 under the Securities Exchange Act of 1934, as amended (the “Exchange Act”). As
a result of the Merger, we have ceased to be a “shell company.”
In connection with
the Merger and under the terms of the Merger Agreement:
||at the effective time of the Merger (the “Effective Time”) each ordinary share of Wize Israel that was issued and outstanding was automatically cancelled and converted into 4.1445791236989 shares of our Common Stock (the “Exchange Ratio”) (not adjusted for the Reverse Stock Split). As a result, an aggregate of 3,915,469 shares of our Common Stock were issued to former Wize Israel shareholders. Our pre-Merger stockholders retained an aggregate of 435,052 shares of our Common Stock;|
||a convertible loan (the “2016 Convertible Loan”) entered into between Wize Israel and Rimon Gold entered into on March 20, 2016 (as amended on March 30, 2016 and December 21, 2017, the “2016 Loan Agreement”) in the principal amount of $531,067 was adjusted based on the Exchange Ratio and became convertible into shares of our Common Stock at a conversion price of $0.9768, subject to adjustments for stock splits and similar events set forth in the 2016 Loan Agreement;|
||a convertible loan (the “2017 Convertible Loan”, and together with the 2016 Convertible Loan, the “Convertible Loans”) entered into between Wize Israel and Ridge Valley Corporation (“Ridge”), and, by way of entering into assignments and assumption agreements following such date, also with Rimon Gold Assets Ltd. (“Rimon Gold”)and Shimshon Fisher (“Fisher,” and together with Ridge and Rimon Gold, the “2017 Lenders”), entered into on January 15, 2017 (as amended on December 21, 2017, the “2017 Loan Agreement”) in the principal amount of $822,144, was adjusted based on the Exchange Ratio and became convertible into shares of our Common Stock at a conversion price of $1.1112, subject to adjustments for stock splits and similar events set forth in the 2017 Loan Agreement;|
||under the 2016 Loan Agreement, as modified by the 2017 Loan Agreement, Rimon Gold has the right, until June 30, 2019, to invest up to $796,601, in the aggregate, at an agreed price per share (as adjusted based on the Exchange Ratio and the 2017 Loan Amendment) of $1.308, if we conduct any equity financing (which condition was met in full upon the closing of the 2017 PIPE (as defined below));|
||under the 2017 Loan Agreement, the 2017 Lenders, have the right until June 30, 2019, to invest up to $411,072, in the aggregate, at an agreed price per share (as adjusted based on the Exchange Ratio and the 2017 Loan Amendment) of $1.332;|
||Wize Israel undertook to cause us to issue, to investors in a private placement of Wize Israel that was completed in July and August 2017, warrants to purchase (as adjusted based on the Exchange Ratio) an aggregate of 904,036 shares of our Common Stock at an exercise price of $1.9728 (the “PIPE Warrants”), which PIPE Warrants were granted on November 16, 2017;|
||immediately prior to the Effective Time, we sold on an “as is” basis to Can-Fite all the ordinary shares of Eyefite, in exchange for the irrevocable cancellation and waiver of all indebtedness owed by us and Eyefite to Can-Fite, including approximately $5 million of deferred payments owed by us and Eyefite to Can-Fite and, as part of the purchase of Eyefite, Can-Fite also assumed certain accrued milestone payments in the amount of $175,000 under the Can-Fite License Agreement. In addition, that certain exclusive license of Can-Fite’s CF101 drug candidate for the treatment of ophthalmic diseases granted to us and the Eyefite Services Agreement was terminated pursuant to a Termination of License Agreement and a Termination of Services Agreement that was entered into on the Closing Date;|
||immediately following the Effective Time, Ron Mayron, Yossi Keret, Dr. Franck Amouyal and Joseph Zarzewsky were appointed to our Board of Directors to hold office until the earlier of the next annual meeting where directors will be appointed, such director’s successor is elected and qualified, or until such director’s earlier resignation or removal and following those appointments, Pnina Fishman, Ph.D. Ilan Cohen, Ph.D., Guy Regev and Roger Kornberg, Ph.D. resigned from our Board of Directors. Accordingly, our Board of Directors consists of five members, Ron Mayron, Yossi Keret, Dr. Franck Amouyal, Joseph Zarzewsky and Dr. Michael Belkin;|
||immediately following the Effective Time, Pnina Fishman, Ph.D., Itay Weinstein and Ronen Kantor resigned as our officers and the newly constituted board appointed Or Eisenberg as Acting Chief Executive Officer, Chief Financial Officer, Treasurer and Secretary and Noam Danenberg as Chief Operating Officer; |
||our Common Stock continued to be quoted on the OTC Pink under the new trading symbol “WIZP” until January 4, 2018, when we commenced trading our Common Stock on the OTCQB; and|
||Wize Israel ordinary shares were delisted from the TASE and there was no longer a public trading market for Wize Israel ordinary shares. |
the completion of the Merger, our pre-Merger stockholders continued to hold 435,052 shares, or 10% of our issued and outstanding
Common Stock, and former Wize Israel shareholders own 3,915,469 shares, or 90% of our issued and outstanding Common Stock (both
percentages excluding (i) shares of Common Stock issuable upon the exercise of the Convertible Loans, (ii) shares of Common Stock
issuable upon the exercise of the Investment Rights (such term is defined on page 67 of this Annual Report), (iii) shares of Common
Stock issuable upon the exercise of the PIPE Warrants, and (iv) shares of Common Stock issuable upon the exercise of certain options
held by our pre-Merger directors and officers (the “Wize Stock Options”). In the event all the Convertible Loans,
Investment Rights, PIPE Warrants and Wize Stock Options were to be exercised in full, then our pre-Merger stockholders and option
holders would own 439,948 shares, and their combined ownership percentage would be reduced to approximately 5.4% of our issued
and outstanding Common Stock, and the former Wize Israel shareholders and holders of Convertible Loans, Investment Rights, PIPE
Warrants and Wize Stock Options on a combined basis would own 7,750,560 shares, or approximately 94.6% of our issued and outstanding
Common Stock, assuming, for the purposes of this calculation, a total of 8,190,508 shares of our Common Stock issued and outstanding
on a fully diluted basis.
As a result of
the Merger, the business of Wize Israel became our ongoing business.
The Merger was accounted for as a reverse
recapitalization of us by Wize Israel. Under reverse recapitalization accounting, our assets and liabilities will be recorded,
as of the completion of the Merger, at their historical amounts. Consequently, the annual consolidated financial information of
Wize Israel for the year ended December 31, 2017 reflects the operations of the acquirer for accounting purposes together with
a deemed issuance of shares, equivalent to the shares held by the former stockholders of the legal acquirer and a recapitalization
of the equity of the accounting acquirer. The annual consolidated financial information includes the accounts of Wize Israel since
inception and our accounts since the effective date of the reverse recapitalization.
On March 5, 2018, we effected the Reverse
The following is a historical background
and corporate history of Wize Israel prior to the Merger:
Wize Israel’s legal and commercial
name is Wize Pharma Ltd. It was formed under the laws of the State of Israel as a company limited by shares on June 23, 1982, under
the name Eitam Eretz Israel Advanced Industries Ltd. In November 1997, Wize Israel changed its name to Orlil Holdings (1982) Ltd.
and in June 2011, Wize Israel changed its name to Star Night Technologies Ltd. In July 2015, Wize Israel changed its name to its
In June 1982, Wize Israel completed its
initial public offering in Israel and its ordinary shares began trading on the TASE. Prior to the Merger, Wize Israel’s ordinary
shares were traded on the TASE under the symbol “WIZP”. From inception until February 2015, Wize Israel engaged in
various businesses and in February 2015 Wize Israel became a public shell company.
In December 2014, an Israeli court approved
a creditors arrangement (the “Creditors’ Arrangement”) under the Israeli Companies Law between Wize Israel (then
known as Star Night Technologies Ltd.), its creditors and its shareholders, in which Wize Israel was purchased by a group of investors
led by Ridge. Upon the completion of the Creditors’ Arrangement, all of Wize Israel’s assets, rights and obligations
were transferred to the creditors’ arrangement fund, so that Wize Israel’s equity after the approval of such arrangement
was zero and Wize Israel remained a public shell company without any activity, rights or obligations. The Creditors’ Arrangement
was completed in February 2015.
Below is a summary of the major business
developments in Wize Israel following the completion of the Creditors’ Arrangement and prior to the Merger:
||On May 1, 2015, Wize Israel entered into
an Exclusive Distribution and Licensing Agreement with Resdevco Ltd. (“Resdevco”), as amended and supplemented
thereafter (the “LO2A License Agreement”), whereby Resdevco granted to Wize Israel an exclusive license to
purchase, market, sell and distribute LO2A in the United States, Israel and Ukraine as well as a contingent right to do the
same in other countries. For more information about the LO2A License Agreement, see under “- LO2A License
Agreement,” beginning on page 8 of this Annual Report. |
||Between April 2015 and August 2017, Wize Israel
entered into a series of equity and debt financings, raising a total of approximately NIS 12.6 million (approximately $3.7
million). For more information about these financings, see Item 7 - “MANAGEMENT’S DISCUSSION AND ANALYSIS OF
FINANCIAL CONDITION AND RESULTS OF OPERATIONS,” beginning on page 62 of this Annual Report.|
||In August 2016, Wize Israel commenced a Phase II, randomized, double-blind, placebo-controlled, clinical trials to evaluate the safety and efficacy of LO2A for patients suffering from moderate to severe CCH.|
Our corporate headquarters are located in
Hod Hasharon, Israel. Our telephone number is +972-72-2600536, and our website is located at www.wizepharma.com. This
website is an inactive textual reference only and not an active hyperlink. The information on or that can be accessed through our
website is specifically not incorporated by reference into this Annual Report, and is not a part of this Annual Report.
The Market Opportunity
We (through Wize Israel) have licensed certain
rights to purchase, market, sell and distribute LO2A for the treatment of DES and other ophthalmological illnesses, including CCH
and Sjögren’s in the United States, Israel, Ukraine, China and have an option to purchase the rights to additional territories
as further described in the LO2A License Agreement below.
Dry Eye Syndrome: DES is an
eye disease caused by eye dryness, which, in turn, is caused by either decreased tear production or increased tear film evaporation.
The tear film is comprised of the lower mucous layer which helps the tear film adhere to the eyes, a middle layer of water
and an upper oil layer that seals the tear film and prevents evaporation. The tear film keeps the eye moist, creates a smooth
surface for light to pass through the eye, nourishes the front of the eye and provides protection from injury and infection. DES
is usually caused by aqueous tear deficiency, or inadequate tear production, whereby the lachrymal gland, the gland that secretes
the aqueous layer of the tear film, does not produce sufficient tears to keep the entire conjunctiva, or the tissue inside the
eyelids that covers the sclera, and cornea covered by a complete layer of tear film. In rare cases, aqueous tear deficiency may
be a symptom of collagen vascular diseases, including rheumatoid arthritis, Wegener’s granulomatosis, an incurable form of
vasculitis (the inflammatory destruction of blood vessels), systemic lupus erythematosus, an autoimmune connective tissue disease,
Sjögren’s, an autoimmune process in which patients suffer from mouth and eye dryness, and autoimmune diseases associated
with Sjögren’s. DES can also be caused by abnormal tear composition resulting in rapid evaporation or premature destruction
of tears. Additional causes include, but are not limited to, age, use of certain drugs and the use of contact lenses.
DES is characterized by eye irritation symptoms,
blurred and fluctuating vision, tear film instability, increased tear osmolarity and ocular surface epithelial disease. DES
causes constant ocular discomfort, typically dryness, burning, a sandy-gritty eye irritation and a decrease in visual function.
Over an extended period of time, DES can lead to tiny abrasions on the surface of the eyes. In advanced cases, the epithelium
undergoes pathologic changes, namely squamous metaplasia, a non-cancerous change of surface-lining cells, and loss of goblet cells,
which secrete mucin, which in turn dissolves in water to form mucous. Some severe cases result in thickening of the corneal surface,
corneal erosion, epithelial defects, corneal ulceration (sterile and infected), corneal neovascularization, or excessive ingrowth
of blood vessels, corneal scarring, corneal thinning, and even corneal perforation. In the most severe cases, DES may result
in deterioration of vision.
In a Market Scope Dry Eye Report (the “Market
Scope Report”), it was estimated that in 2016, approximately 344 million people around the world suffered from various levels
of DES and Market Scope expects the global dry eye treatments market to total $3.7 billion in 2017 and to reach $4.9 billion in
2022. According to the Market Scope Report, the factors that contribute to the increase in the number of those suffering from
DES include the extended viewing of television, computer and Smartphone screens, weather conditions, exposure to air conditioning
and increased life expectancy. According to the abovementioned report, the global DES treatments market is expected to grow at
a compounded annual growth rate of 5.5 percent, reaching $4.5 billion in 2021. The highest
rate of growth is expected to occur in China, India, and other emerging markets where they forecast double-digit compounded annual
growth rates due to aging populations, increasing wealth, and improving access to health care.
Conjunctivochalasis: CCH refers to
the presence of redundant folds of loose conjunctiva. CCH is thought to be caused by both a gradual thinning and stretching of
the conjunctiva that accompanies age and a loss of adhesion between the conjunctiva and underlying sclera due to the dissolution
of Tenon’s capsule. A correlation may also exist between eye inflammation and CCH, though it is unclear if this correlation
is causal. CCH may also be associated with previous surgery, blepharitis, Meibomian gland disorder, Ehlers-Danlos Syndrome and
aqueous tear deficiency. The resulting loose, excess conjunctiva may mechanically irritate the eye and disrupt the tear film and
its outflow, leading to dry eye and excess tearing. Most patients with CCH complain of foreign body sensation, tearing, difficulty
reading, blurred vision, “red eyes” and general irritation.
Lid Parallel Conjunctival Folds (“LIPCOF”)
grading measures the number and severity of the lid-parallel conjunctival folds. LIPCOF grade 0 signifies the absence of conjunctival
folds, LIPCOF grade 1 signifies just one conjunctival fold, LIPCOF grade 2 signifies for multiple conjunctival folds, not extending
beyond the tear meniscus, and LIPCOF grade 3 signifies multiple conjunctival folds extending above the tear meniscus. The LIPCOF
grades show a strong correlation with both the subjective and objective complaints of DES, as well as with the severity of the
The treatment of LIPCOF grade 3 CCH usually
requires invasive therapies like surgery or treatment of the conjunctival folds with argon laser or with heat cauterization. A
previous study conducted by Resdevco in 2013, has shown Conheal® (Hungarian brand name for LO2A) to be effective
in reducing the severity of CCH as measured by a reduction in the (i) LIPCOF score, (ii) Oxford scheme grade and (iii) ocular surface
disease index (“OSDI”) and an increase in tear film break-up time (“TFBUT”). This raises the possibility
that vision-related quality of life can be significantly improved by conservative therapies even in severe CCH.
is little epidemiological data for CCH. A community based study in Shanghai reported that in patients over the age of 60, 4% had
LIPCOF grade 3 CCH and 16% had LIPCOF grade 2
CCH. In the European Union, about 20% of the population is over the age of 65. From the aforementioned data, it might be assumed,
as presented in a study conducted by Dr. Huba J. Kiss and János Németh, that in the total European Union population,
0.8% have LIPCOF grade 3 CCH and 3.2% have LIPCOF grade
2 CCH. Since DES complaints occur in 5.5% to 33.7% of the population, Dr. Kiss and Németh further assumed that the incidence
of the CCH-caused DES in the population is about one-third of all DES cases.
Sjögren’s syndrome: Sjögren’s
syndrome is a heterogeneous, chronic, inflammatory, autoimmune disease characterized by lymphocytic infiltration of exocrine glands
and expression of autoantibodies including antinuclear antibody (ANA), anti-Ro (also termed anti SSA), anti-La (also termed anti
SSB) as well as rheumatoid factor (RF). Hypergammaglobulinemia is common as well. Sjögren’s may be an isolated disease,
termed primary Sjögren’s syndrome or may accompany another autoimmune diseases, such as lupus, rheumatoid arthritis,
or scleroderma, thus termed secondary Sjögren’s syndrome. Clinical presentation varies from mild symptoms such as classic
sicca symptoms of dry eyes (xerophthalmia), dry mouth (xerostomia) and parotid gland enlargements to severe systemic symptoms involving
multiple organ systems such as fever, fatigue, malaise, arthritis, arthralgia, myalgia, interstitial lung disease, kidney disease,
gastrointestinal disease and neurological manifestations. Sjögren’s treatment is highly individualized and is based
on a patient’s disease severity, organ involvement and previous response. Mild forms of Sjögren’s may be treated
symptomatically with artificial tears and salivary flow stimulation. More severe, systemic manifestations may be treated with high-dose
glucocorticoids and immunosuppressive or cytotoxic drugs to suppress the immune system.
Estimations of Sjögren’s prevalence
vary from 2.5 million to 4 million patients (Sjögren’s Syndrome Foundation) in the US alone, with a worldwide estimate
of up to 7.7 million in the 7 Major Markets (US, France, Germany, Italy, Spain, the UK and Japan) by the year 2024 (Global Data
Research). Sjögren’s affects mostly middle aged women (40-50 years of age) with a female to male prevalence ratio of
Global Data estimates the drug sales for
Sjögren’s in 2014 were approximately $1.1 billion across the markets covered in its forecast. By the end of the forecast
period of 2024, sales are estimated to grow to $2.2 billion across the markets covered in its forecast with a Compound Annual
Growth Rate of 7.2%. The market size estimate in 2014 includes Salagen (pilocarpine) and Evoxac (cevimeline), the only two agents
to ever be approved for Sjögren’s, and the use of off-label agents, such as biologics approved for other autoimmune
diseases, and systemic and topical immunosuppressants and corticosteroids. This growth is expected to be driven by the anticipated
approval of Orencia for use in patients with Sjögren’s in the US and EU in 2021 and Japan in 2022.
LO2A License Agreement
The following summary of the LO2A License
Agreement as well as all summaries of agreements provided herein are qualified to the full text of the agreements, which are filed
as exhibits hereto.
In May 2015, Wize Israel entered into the
LO2A License Agreement with Resdevco, a company controlled by Professor Shabtay Dikstein, the inventor of LO2A. Pursuant to the
LO2A License Agreement, Resdevco granted to Wize Israel (and thereafter, to OcuWize Ltd. (“OcuWize”), Wize Israel’s
wholly owned subsidiary, as described below) an exclusive license to develop in the United States, Israel and Ukraine, under the
LO2A licensed technology, products in the field of ophthalmic disorders, and to mutually agree upon a manufacturer and to purchase,
market, sell and distribute LO2A in finished product form in the Licensed Territories in the field of ophthalmic disorders. Subject
to certain limited exceptions, Wize Israel may not sublicense or sell or transfer any of its rights under the LO2A License Agreement
without the advance written approval of Resdevco.
The LO2A License Agreement grants Wize Israel
the right to add additional territories in the future, subject to a commitment by Wize Israel to pay minimum royalties according
to a formula set forth in the LO2A License Agreement with respect to the additional territory, and provided that Resdevco has not
granted exclusive rights in such additional territory or is in ongoing negotiations. The LO2A License Agreement also grants Wize
Israel the right to purchase Resdevco’s agreements with its existing distributors of LO2A in other jurisdictions (namely,
Germany, Hungary, Netherlands and Switzerland (collectively, the “Reserved Territories”) for ten times the greater
of the net royalties received in the previous 12 months under such agreements or the minimum royalty payment under such agreements.
The LO2A License Agreement furthermore grants Wize Israel a right of first negotiation with potential distributors to whom Resdevco
may in the future grant distribution rights to LO2A outside of the Reserved Territories and the Licensed Territories and provides
that if Wize Israel enters into such distribution agreement in accordance with the LO2A License Agreement, then Wize Israel has
agreed to guarantee in writing to Resdevco that it will pay to Resdevco minimum royalties according to a formula set forth in the
LO2A License Agreement. The LO2A License Agreement historically included an option to purchase all remaining territories for a
fixed amount and such option was cancelled on March 30, 2017.
The LO2A License Agreement provides that
Wize Israel is required to pay to Resdevco certain royalties for sales in the Licensed Territories based on an agreed-upon price
per unit payable on a semi-annual basis, subject to making certain minimum royalty payments, which (1) with respect to the United
States, means the non-refundable and non-deductible aggregate amount of $400,000 over a period of three years commencing from 2015
(which amount was already fully paid by Wize Israel) and an advance against royalties of $475,000 per year starting January 1,
2018 (which Resdevco agreed to reduce to $150,000 for January 1, 2018 and January 1, 2019, with the understanding that if Wize
Israel obtains an FDA marketing license in 2019, then Wize Israel will pay Resdevco the remaining 2019 payment of $325,000 within
30 days of the receipt of such FDA license), which annual advance shall be credited towards any royalties payable to Resdevco for
that particular year, (2) with respect to Israel, means an upfront non-refundable and non-deductible payment of $30,000, payable
at commencement of local sales, and an annual advance against royalties starting January 1, 2017 in increasing payments depending
on the year (up to a maximum of $36,000) which annual advance shall be credited towards any royalties payable to Resdevco for that
particular year, and (3) with respect to Ukraine, means an annual advance against royalties, starting in 2016, in increasing payments
depending on the year (up to a maximum of $30,000), which yearly advance shall be credited towards any royalties payable to Resdevco
for that particular year.
On January 5, 2017, Wize Israel and Resdevco
entered into an amendment to the LO2A License Agreement, pursuant to which the payment of $150,000 that Wize Israel was obligated
to pay to Resdevco on January 1, 2017, was postponed to March 31, 2017. On March 30, 2017, Wize Israel and Resdevco entered into
a second amendment to the LO2A License Agreement, pursuant to which the payment of $150,000 was further postponed to May 31, 2017.
In the end of May 2017, the parties agreed to postpone the aforementioned payment to the beginning of July 2017, when the payment
was made. In the end of December 2017, Resdevco notified Wize Israel that the minimum royalty payment with respect to the United
States would be postponed until January 20, 2018 and in January 2018, Resdevco agreed to postpone such payment until July 29, 2018.
The LO2A License Agreement has an initial
term of seven years that expires in May 2022, and, unless Wize Israel provides prior notice of at least 12 months terminating the
agreement, the LO2A License Agreement renews automatically each year. Wize Israel may terminate the LO2A License Agreement prior
to May 2022 upon 180 days prior notice; provided that all payments previously made to Resdevco shall be non-refundable, any payments
due during the 180 day notice period shall be payable to Resdevco and Wize Israel is required to pay a penalty of $100,000, depending
on the timing of termination. Additionally, if Wize Israel terminates the LO2A License Agreement, it is required to exert reasonable
best efforts to find a third party willing to sell LO2A under the same terms as the LO2A License Agreement. The LO2A License Agreement
may be terminated by either party upon the occurrence of certain other customary termination triggers, including material breaches
of the LO2A License Agreement by either party, as well as the right of Resdevco to terminate the LO2A License Agreement (or halt
the manufacturing agreement or cease delivery of any finished product for any period of time) as a result of Wize Israel not paying
all royalties due under the LO2A License Agreement. In addition, Resdevco may terminate the LO2A License Agreement, upon 30 days
written notice, if (1) an application for the marketing approval of LO2A, for the treatment of DES is not submitted to the FDA
or the equivalent regulatory authority in the Licensed Territories by May 1, 2019, (2) such FDA approval is not obtained from the
FDA or the equivalent regulatory authority in the Licensed Territories by May 1, 2021, (3) such approval has been obtained, commercial
sales of LO2A have not commenced within three months thereafter, (4) commercial sales of LO2A have commenced, any royalties, including
any minimum royalties are not timely paid, or (5) Wize Israel attempts to sell competing products in or outside the Licensed Territory.
Resdevco may also terminate the LO2A License Agreement if Wize Israel contests the validity of any patents covering LO2A or any
related know-how or if Wize Israel makes, sells or exploits a competing product to LO2A.
The LO2A License Agreement contains other
provisions, including representations and warranties of the parties, reporting, confidentiality and other covenants, such as an
undertaking by Wize Israel not to sell competing products in the Licensed Territories during the term of the agreement and for
five years thereafter. The LO2A License Agreement further provides that any improvements or modifications made by Wize Israel to
LO2A or any related intellectual property or know-how shall belong to Resdevco and Wize Israel shall receive a license to distribute
and sell the same in the Licensed Territories on the same terms set forth in the LO2A License Agreement.
In order to secure Wize Israel’s
obligations and performance pursuant to Convertible Loans made by Rimon Gold, Wize Israel’s rights under the LO2A License
Agreement serve as collateral. For details related to those security interests, see Item 7 - “MANAGEMENT’S DISCUSSION
AND ANALYSIS OF FINANCIAL CONDITION AND RESULTS OF OPERATIONS,” beginning on page 62 of this Annual Report.
In August 2016, Resdevco granted Wize Israel
an option to purchase its ownership rights to LO2A, including the patents and trademarks thereunder, except in countries in which
LO2A is already sold by Resdevco. In accordance with the terms of this option, Wize Israel was required to pay for such ownership
rights a non-recurring payment of $440,000 as well as royalties from future sales of LO2A and to issue an option to purchase 41,667
of its ordinary shares. This option expired on December 31, 2016 and Wize Israel and Resdevco are currently negotiating the terms
of a new option for Wize Israel to purchase certain rights of LO2A.
In August 2016, Wize Israel and Resdevco
also entered into an agreement pursuant to which Wize Israel assigned all of its rights and obligations under the LO2A License
Agreement to OcuWize.
On September 6, 2017, Resdevco granted to
Wize Israel, sole rights to commercialize LO2A in China. By agreement dated September 25, 2017, Wize Israel and Resdevco agreed
that Wize Israel’s sold rights to commercialize LO2A in China shall be limited to one year if by September 6, 2018, Wize
Israel has not signed a distribution agreement for LO2A in China.
On December 26, 2017, Wize Israel, entered
into an amendment to the LO2A License Agreement (the “Third Amendment”). The Third Amendment includes: (i) China in
the list of Licensed Territories, (ii) the commercial terms of the parties with respect to the activities of Wize Israel in China,
including the minimum annual royalty payments from Wize Israel to Resdevco, and, (iii) an undertaking by Wize Israel to include
in the distribution agreement to be entered into with the Chinese Distributor that the Chinese Distributor will transfer the Chinese
market license to Resdevco upon termination of the distribution agreement. In the event Wize Israel fails to execute a distribution
agreement with the Chinese Distributor by June 1, 2018, the Third Amendment will be deemed null, void and of no force.
On January 8, 2018, Wize Israel entered
into a Memorandum of Understanding (the “MOU”) with Resdevco. Pursuant to the MOU, Resdevco granted to Wize Israel
(and its permitted assignees) an exclusive royalty bearing license to sell and distribute worldwide (excluding the United States,
Israel, Ukraine, Switzerland, Germany, Netherlands and, subject to certain conditions, China, the “Additional Territories”),
under the LO2A licensed technology, products in the field of ophthalmic disorders, under the terms and conditions set forth in
the MOU, including the following: (i) the license for each Additional Territory shall be conditional on signing a specific license
agreement for each Additional Territory that shall include the basic terms and conditions set forth in the MOU, including reaching
minimum sales targets in such Additional Territory pursuant to a formula set forth in the MOU; (ii) for each Additional Territory,
both Wize Israel and the local distributor shall be responsible to pay Resdevco a minimum per product fee in accordance with a
formula set forth in the MOU and the agreement with the distributor shall be subject to Resdevco’s prior approval (which shall
not be unreasonably withheld); (iii) if Resdevco introduces Wize Israel to a distributor in any Additional Territory, Wize Israel
will enter good faith negotiations with such distributor and, if Wize Israel does not reach an agreement with such distributor,
Resdevco may enter into a distribution agreement with such distributor, in which case, Wize Israel will provide the services it
typically provides to its other distributors in consideration for a portion of the royalties payable to Resdevco; and (iv) the
license granted under the MOU is for an initial term of 5 years and, thereafter, automatically renews for additional terms of 5
years each, subject to full compliance with the terms set forth in the MOU and as long as the LO2A License Agreement is in effect.
The MOU also provides that it shall be in effect until a definitive agreement reflecting the terms of the MOU is executed, which
the parties committed to exercise their best efforts to do within three months.
LO2A is a drug developed by Prof. Dikstein
in the 1990s, initially for the treatment of DES, and later on for other ophthalmological disorders, including CCH and Sjögren’s.
LO2A is a sterile, preservative-free, single-dose artificial tear preparation containing 0.015% sodium hyaluronate (“SH”)
as the drug substance. It has been developed as a substitute for natural tears, in order to lubricate and protect the ocular surface
SH is a salt of hyaluronic acid (“HA”).
HA is present in the extracellular matrix (“ECM”) of all tissues and is particularly abundant in vitreous humour, skin,
cartilage and the synovial fluid of joints. HA’s long chain molecules form a filter matrix interspersed with cellular fluids,
which provide visco-elastic properties to the tissues. In the eye, endogenous HA forms a layer over the surface of the cornea.
It serves to protect the corneal cells and reduce cell damage; so it is important in maintaining cell viability.
HA is an important pericellular and cell-surface
constituent and is involved in the regulation of cellular activity through its interaction with other macromolecules. Recently,
nonclinical pharmacological experiments have shown that HA promotes the viability of corneal cells and corneal epithelial wound
healing by direct interaction with cell receptors. It acts as a signaling molecule in the ECM and is a ligand for specific receptor
molecules, notably CD44, a cell surface adhesion molecule found on human corneal cells. Increased expression of CD44 receptors
has been shown to be associated with corneal re-epithelialization. Any disruption of corneal integrity, as may occur with dry eyes,
triggers the re-synthesis of HA and increases cell proliferation. These effects have been demonstrated to be dose-dependent.
LO2A eye drops incorporate a high molecular
weight SH (1.5-1.65 million Da), which enables it to be effective in solution at a low concentration. It confers specific physical
properties upon a solution. Its complex molecular structure, adsorbs a relatively high volume of water, so that the solution takes
on a gelatinous form. This water is released upon an increase in pressure. The viscosity of high MW SH is affected by shear rate;
at high shear rate the macromolecules change their shape, align in the treatment of flow and its viscosity decreases. This enables
the LO2A solution to flow across the corneal surface immediately after blinking. The physiochemical property of SH is similar to
that of mucin, which constitutes the base layer of the lacrimal film and interacts strongly with the corneo-conjunctival surface.
Molecules of mucin are able to bind water molecules up to 80 times greater in weight than their own. This is due to a large number
of negatively-charged glycoside groups that are attached to the terminal section of the polypeptide skeleton.
All excipients included in LO2A eye drops
comply with the relevant monographs of the European Pharmacopoeia. None of the excipients are of animal or human origin. They are
established excipients for pharmaceutical products, including those approved for ocular use. Their functions include adjusting
tonicity and increasing the viscosity of the formulation. This allows the LO2A eye drops to have a lubricating effect that is compatible
with the external ocular environment. The visco-elasticity of LO2A eye drops ensures that they are retained on the corneal surface
for a period of 4-6 hours, as demonstrated in a Phase I clinical pharmacology study conducted with LO2A in the University Hospital
of Antwerp, Belgium in 1992. In this Phase I, randomized, blinded, cross-over study, fluorescence was used to measure pre-corneal
retention time in healthy volunteers following a single instillation of LO2A and placebo (isotonic phosphate buffered saline) both
labeled with fluorescein. The study compared the elimination coefficient and area under fluorescence decay curve for LO2A versus
LO2A eye drops do not contain any preservatives.
This is an important feature of the formulation as preservatives have a recognized potential for irritation and sensitization and
can damage the ocular surface and the cornea. This is of particular relevance to patients with symptoms of DES, in whom the corneal
surface is already compromised.The adverse events reported both from clinical trials of LO2A and from literature reports of different
eye drop formulations containing SH, were minor ocular events which are expected to occur with any ophthalmic formulation. LO2A
eye drops are presented in sterile, unit-dose vials to minimize the risk of infection and contamination.
We believe that the properties of the LO2A
formulation described above make it a suitable candidate for use in a variety of dry eye indications including those with an inflammatory
component. LO2A is currently registered and marketed in Germany and Switzerland for the treatment of DES, in Hungary for the treatment
of DES and CCH and in the Netherlands for the treatment of DES and Sjögren’s. LO2A is sold under the brand name Hylan®
in Germany and the Netherlands, Lacrycon® in Switzerland, and Conheal® in Hungary. LO2A has been
sold by Resdevco through local distributors in these countries for a number of years. In these countries, the drug is sold in a
unit dose format, and is manufactured in Germany and France. We currently intend to market LO2A as a treatment for DES, CCH and
Sjögren’s in the Licensed Territories, and believe that LO2A for treatment of ophthalmic inflammatory disorders such
as CCH and Sjögren’s presents a significant market opportunity.
We intend to distribute LO2A via local or
multi-national distributors, including by cooperation with a major medical company with means and experience in the end processes
of approving and marketing drugs. In order to register LO2A for the treatment of dry eye patients suffering from CCH and Sjögren’s,
we estimate that LO2A will be required to undergo additional clinical trials in addition to the Phase II clinical trial that we
are currently conducting.
The following paragraphs describe the non-clinical
and clinical data upon which approvals were granted.
A summary of the toxicology studies conducted
on LO2A and the drug substance is provided in Table 1 below. The acute and sub-acute toxicity studies conducted with the drug substance
and LO2A demonstrated a low order of toxicity. This is in-line with published reports of acute toxicity studies conducted with
SH administered to rodents and other species, including beagle dogs. Similarly, literature reports of sub-acute and chronic toxicity
studies conducted in a wide range of species using different exposure routes, including ocular application, have repeatedly demonstrated
that it did not cause significant toxic effects.
The systemic absorption of SH is clinically
negligible and published reproductive and developmental toxicity tests have demonstrated that it does not cause any teratogenic
effects or adverse effects on reproduction. Animal studies have shown that it is secreted into breast milk after parenteral injection,
but no adverse effects were caused in the young.
Ocular tolerance studies have been conducted
with the drug substance and LO2A solution. Sodium hyaluronate was found to cause mild irritation when applied in powder form to
the eyes of rabbits; the signs of irritation were more frequent and more severe in the group that did not receive eye irrigation
immediately after instillation. In such studies, no other macroscopic ocular findings were reported. A further 28-day study of
the primary eye irritation of LO2A solution in rabbits caused mild ocular irritation; all other ocular and systemic investigations
revealed no adverse effects. In both of these studies all signs of irritation had resolved within 48 hours. Application of the
concentrated drug substance would be expected to cause a degree of non-specific irritation, by virtue of its physical presence
in the eye.
After instillation of eye drops, there is
inevitably a degree of spillage onto surrounding skin. Therefore, a standard skin sensitization study was conducted on LO2A. This
demonstrated that it had no sensitization potential. This is in-line with published reports of skin irritation and sensitizing
studies conducted in guinea pigs and rabbits.
The drug substance was shown not to be mutagenic
in a bacterial mutation test. Published reports of the chromosome aberration and mouse micronucleus tests confirm that it is not
mutagenic or genotoxic. No carcinogenicity testing has been conducted, but SH has well-established safety for long-term use.
Table 1: List of Toxicology Studies Performed During the
Development of LO2A / Sodium Hyaluronate
||Clinical observation Body Weight
||LDLo > 1500 mg/kg.|
|New Zealand Albino Rabbits
||One drop LO2A 6x daily to right eye
||One drop NaCl 0.9% 6x daily to left eye
||Clinical observation Food consumption Body weight Clinical hemistry / Haematology Autopsy / Organ weights / Histology Ocular macroscopic examination (Draize) Slit Lamp eye examination/visual reflexes
||No abnormalities detected in tests conducted; Ocular examinations showed good tolerance to LO2A.|
|Japanese White Albino Rabbits
||Lower Conjunctival Sac
||15.7 mg sodium hyaluronate to right eye; in 3 rabbits followed by 30s irrigation with distilled water
||No treatment to left eye
||Clinical observation Body weight Ocular macroscopic examination (Draize)
||Weak, reversible irritation observed.|
||Induction (I):Intra-dermal injection + Challenge (C): Topical with closed patch
||0.05 ml (1.5%)
||Vehicle (distilled water) Positive control (DNCB) + Vehicle (Olive oil)
||Day 0 (I) - Day 7 (C) + 48hrs
||Body weight Dermal reaction scores at 24 and 48hr after Challenge
||Dermal reactions noted in DNCB group only.|
|Salmonella typhirium TA: 98, 100, 535, 1537; Escherichia coli WP2 uvrA
||Aroclor-induced rat liver S9-mix
||Positive: 2-(2-Furyl)-3-(5-nitro-2-furyl)acrylamide, NaN3, N-Ethyl-N’-nitro-N-nitrosoguanidine, 9-Aminoacridine, 2-Aminoamthracene and Benz(a)pyrene Negative: Purified Water
||62.5 - 1000μg/plate (highest tested concentration due to high viscosity of sodium hyaluronate) Experiment repeated x 2 Cultures replicated x 2
||Cytotoxic: No bacteriostatic effect|
Genotoxic effect: No significant increase of the number of revertants against negative control
Effect of positive control: High number of revertants.
A pivotal clinical trial conducted with
LO2A eye drops in six centers in France, is summarized below. There are a further seven published clinical studies on LO2A, which
are also summarized. Six of these studies documented the efficacy of LO2A eye drops by both the Investigators and the patients.
Adverse events and tolerance parameters were also recorded. The remaining study specifically investigated tolerance parameters
after application of LO2A eye drops. No clinical Pharmacokinetics studies have been conducted for LO2A eye drops. The PK profile
of SH is well established. Extensive safety monitoring in both animal and human studies have shown that, after ocular application,
no clinically meaningful systemic absorption is expected.
A Phase I study was performed at the University
of Antwerp, Belgium in 1992 to measure the pre-corneal residence time of LO2A eye drops versus placebo in healthy volunteers (Study
EC-914-1B). This was a single blind study in which 6 healthy volunteers received a single administration of LO2A eye drops to one
eye and placebo to the other eye, both labeled with fluorescein. Variance analysis (ANOVA) for the area under the fluorescence
delay curve demonstrated that LO2A was retained on the corneal surface significantly longer than placebo eye drops (p=0.048; significance
level p=0.05). No adverse events were reported.
Six Phase II studies were performed. These
are described below:
Randomized Controlled Trial of High
Molecular Weight Hyaluronic Acid (LO2A) in DES
This study was performed in 1992 at the
Hospital San Biagio, Domodossola, Italy. The objectives of the study were to evaluate the efficacy of 30-day treatment with LO2A
in reducing the severity of DES, to confirm an optimum dosing schedule for LO2A (3, 4, 6 or 8 drops/day) and to assess the interference
of LO2A with other ocular therapies. One hundred patients with moderate-to-severe DES were randomized 1:1 to treatment (LO2A) or
comparator (Hyalistil containing 0.2% SH and the preservative thimerosal at 0.005%). Statistical analyses were performed using
Wilcoxon, Mann-Whitney U test and Chi square test. The significance level was p=0.05.
The study demonstrated significant improvement
in composite score from objective parameters including Schirmer test, fluorescein staining, TFBUT and Rose Bengal staining (p<0.001
for both treatments using Wilcoxon test), but no significant difference between treatment groups in the reduction in total scores
at Day 30 (p=0.998 using Mann-Whitney U test). For LO2A, a dosing schedule of four applications/day reduced scores at Day 30 significantly
more than lower dosing schedules (p=0.02 using Mann-Whitney U test). There was no significant difference between 4 applications/day
and higher dosing schedules. The number of patients rating tolerance as ‘good’ or above was significantly higher for
LO2A (96%) than the comparator (78%)(p = 0.029 using Chi square test). Adverse events were experienced by two patients in the LO2A
group (both “sticky eye”) and 11 patients in the comparator group. There were no serious adverse events (“SAEs”)
or apparent interactions between LO2A and concomitant eye treatments.
Double-Masked, Crossover Comparison of a New
Artificial Tear Preparation containing Hyaluronic Acid (LO2A) and Lacrisol® in DES Treatment
This study was performed in 1992 at the
University of Florence, Italy. The objectives of the study were to compare the efficacy of LO2A with Lacrisol® at
reducing the severity of DES and reducing ocular signs and symptoms. Thirty-five patients with moderate-to-severe DES were treated
alternately with LO2A for a 30-day treatment period and then Lacrisol® for a further 30-day treatment period. The
trial was double-blind and allocation of treatments at Day 0 was randomized. Lacrisol® is an eye drop product containing
0.5% Hydroxypropyl Methylcellulose (“HPMC”). Statistical analyses were performed using Wilcoxon tests. All analyses
were performed using two-sided tests and results were considered to be statistically significant if the p value was less than or
equal to 0.05.
This study demonstrated a statistically
significant improvement in mean, objective dry eye score (based on Schirmer test, fluorescein staining, TFBUT and Rose Bengal staining)
following LO2A treatment compared to the Lacrisol® group (p<0.001). The severity of ocular signs and symptoms
including redness, burning, foreign body sensation and photophobia was significantly less following LO2A treatment (p<0.02 for
photophobia and p<0.01 for other symptoms). Adverse events were experienced by 4 patients treated with LO2A (two patients with
mild burning, one patient with blurred vision and one patient with “thread sensation”) and 10 patients treated with
Lacrisol®. There were no SAEs reported.
Double-Masked Clinical Trial of an
Unpreserved Hyaluronic Acid Based Eye Drops (LO2A) in DES
This study was performed in 1992 at the
University of Genoa, Italy. The objective of the study was to compare the efficacy of LO2A with Lacrisol® in reducing
the severity of DES and ocular symptoms. Twenty-three patients with moderate to severe DES applied LO2A to the first eye and Lacrisol®
(0.5% HPMC) to the second eye. The trial was double-blind and the treatment regime was five applications/day for 30 days. The recorded
data were statistically analyzed by using the Student’s t test and Mann-Whitney U test. The threshold for clinical significance
This study demonstrated that after 30 days
of treatment the mean, objective dry eye scores (based on measurement of meniscal thickness, fluorescein staining, TFBUT and Rose
Bengal staining) for LO2A treatment were significantly lower than for Lacrisol® treatment for three out of the four
tests (p=0.011 for TFBUT [Student t test], p=0.046 for fluorescein staining [Mann-Whitney U test] and p=0.032 for Rose Bengal staining
[Mann-Whitney U test]). The thickness of the lacrimal meniscus did not change significantly in any patient; however, the range
of values recorded at Day 0 (0.1-0.2 mm) was not indicative of pathological changes. The severity of the ocular symptoms (burning,
foreign body sensation and photophobia) was also significantly reduced for LO2A treatment compared to Lacrisol®
at Day 30 (p=0.009 for burning, p=0.006 for foreign body sensation and p=0.025 for photophobia using Mann-Whitney U test). There
were no adverse events associated with LO2A treatment.
Clinical Evaluation of LO2A Eye Drops
versus Reference in Patients suffering from DES
This study was performed in 1992 at the
University of Rome “Tor Vergata”, Italy. The objective of the study was to compare the efficacy of LO2A with eye drops
containing 0.5% HPMC in reducing the severity of DES. Sixteen patients were treated with LO2A or HPMC eye drops. The study was
double blind and assessed the treatment of 5 drops/day for 3-4 weeks. The data were statistically analyzed by comparing the scores
obtained by the Wilcoxon test and adopting a significance threshold of p = 0.05. This study demonstrated that LO2A eye drops had
significantly lower scores than HPMC in the fluorescein (p=0.001), TFBUT (p=0.015) and Rose Bengal test (p=0.007). There was no
difference between treatments in meniscal thickness measurements and Schirmer tests. Adverse events were reported by one patient
treated with LO2A (blurred vision). There were no SAEs reported.
Assessment of Tolerance to LO2A Eye
This study was performed at the University
of Catania, Italy in 1992. The objective of the study was to assess the ocular tolerance of patients with moderate to severe DES
to the application of LO2A drops compared with eye drops containing 0.5% HPMC. Eighteen patients applied LO2A drops to the first
eye and HPMC in the second eye. The study was double-blind and assessed treatment of 4 drops/day for 20 days. This study demonstrated
that 11 out of 18 patients (61.1%) experienced no discomfort upon application of LO2A compared to 1 out of 18 patients (5.6%))
with HPMC eye drops. This difference was found to be highly significant (p=0.0004) according to chi-squared test (significance
level was p=0.05). The subjective symptoms reported at the time of HPMC instillation included blurred vision (16/18; 89%), foreign
body sensation (11/18; 61%), stinging (7/18; 39%), photophobia (2/18; 11%) itching (1/18; 6%) and pain (1/18; 6%). The subjective
symptoms reported at the time of LO2A instillation included foreign body sensation (5/18; 28%), stinging (4/18; 22%), blurred vision
(3/18; 17%) and photophobia (2/18; 11%). No SAEs were reported.
The Effect of a New Tear Substitute
Containing Glycerol and Hyaluronate on Keratoconjunctivitis Sicca
This study was performed in 1998 at Hadassah
University Hospital, Jerusalem, Israel. The objective of the study was to evaluate the efficacy of LO2A in patients suffering from
keratoconjunctivitis sicca compared to their current tear substitute. Twenty-five patients with a history of dry eye symptoms for
at least one year who were using a known tear substitute preparation (containing either cellulose derivatives or polyvinylpyrolidone
plus hydroxyethylcellulose) and had positive Rose Bengal staining were included. One eye was randomized to topical treatment with
LO2A and the other “control” eye to continued treatment with the pre-existing tear substitute preparation. In the first
stage of the study, 15 patients received treatment for one week and in the second stage, 10 patients received treatment for two
weeks. Statistical analysis of the results included the Wilcoxon signed rank test for comparison between scores for the same eye
at different times, and Mann-Whitney test for comparison between scores of study versus control eyes adopting a significance threshold
of p = 0.05.
The average patient satisfaction score for
LO2A was significantly higher compared to the control preparation at 1 week (p=0.0003) and at 2 weeks (p=0.0232). A highly significant
reduction in Rose Bengal staining was demonstrated following one week of treatment with LO2A (p<0.0001) and the LO2A-treated
eyes had significantly less staining compared to control eyes at both one (p=0.021) and two weeks (p=0.023). The paper did not
report any adverse events associated with LO2A treatment.
The pivotal, Phase III study is described
Acceptability and Efficacy of LO2A Eye Drops
vs Gel-Larmes® in Moderate to Severe DES - Clinical Trial Protocol No. EC-921-3
This study was performed in 1993 at the
Hospital Hôtel-Dieu, Paris, France with additional sites in Brest, Montpellier, Limoges, Lyon and Nice. The objective of
this study was to demonstrate the superiority of LO2A to Gel-Larmes® (0.3% Carbomer containing the preservative
thimerosal at 0.005%) in improving patient symptoms and to demonstrate equivalence of the study treatments in reducing the severity
of DES. One hundred patients with moderate to severe DES were randomized 1:1 to treatment (LO2A) or Gel-Larmes®.
The study assessed treatment of four applications/day for 12 weeks. Differences between the study treatment groups were analyzed
statistically using either the Student’s t test (means) or Chi squared test (percentages). Equivalence between the treatment groups
was tested by comparison of distributions using the Dunett and Gent’s Chi squared test. Probability level was 0.05.
This study demonstrated that LO2A was significantly
superior to Gel-Larmes® in improving patient symptoms (p=0.024). The severity of DES was measured using Schirmer
test, fluorescein staining, TFBUT and Rose Bengal staining. A reduction in total score of ≥4, obtained from these four objective
tests, was achieved by 17 patients (left eye) and 23 patients (right eye) in the LO2A group and by 20 patients (left eye) and 16
patients (right eye) in the Gel-Larmes® group, demonstrating that LO2A and Gel-Larmes® were equivalent
in improving signs of DES (probability of equivalence: p=0.039 right eye and p=0.00002 left eye). The number of patients rating
tolerance as ‘good’ or above was significantly higher in the LO2A group compared to Gel-Larmes® at all
time points (Days 15 - p=0.031; Day 45 -p=0.00006; Day 90 - p=0.0004). Adverse events were experienced by 10 patients (21.7%) in
the LO2A group and 17 patients (36.2%) in the Gel-Larmes® group. The adverse events experienced by patients in the
LO2A group included inflammatory reaction (2 patients), burning/itching/stinging sensation (7 patients) and secretions (1 patient).
One unrelated SAE was reported in this study (chest pain) in a patient randomized to the Gel-Larmes® group. In conclusion,
this study demonstrated that LO2A was significantly better than Gel-Larmes® in terms of subjective symptoms and
tolerability in treating DES with a treatment regimen of four drops/day for 12 weeks and equivalent in improving signs of DES.
A Phase II study was performed at Semmelweis
University, Budapest, Hungary between 2012-2013 to assess the efficacy of LO2A eye drops in patients with severe CCH. Twenty patients
with Grade 2 or 3 CCH (according to LIPCOF score), who had previously failed treatment on a variety of artificial tear preparations,
applied LO2A eye drops to both eyes in a single arm, open label study. Patients applied 4 drops/day for each eye for 3 months.
A mean decrease from baseline of one LIPCOF degree was assumed to be clinically relevant. Statistical comparisons were performed
using a paired t-test (TFBUT) or Wilcoxon Signed Rank Test (LIPCOF degree, Oxford grade and OSDI score) at a two-sided significance
level of 5% (p=0.05).
This study demonstrated that after 3 months,
CCH decreased from a mean LIPCOF degree of 2.9±0.4 in both eyes to 1.4±0.6 on the right (median decrease of -2 points,
95% confidence interval (“CI”) from -2.0 to -1.0), and to 1.4±0.7 on the left eye (median decrease of -1 points,
95% CI from -2.0 to -1.0) (p< 0.001 for both sides). The TFBUT increased significantly after one-month treatment (right eye
median increase of 1.1 sec, 95% CI from 0.2 to 1.0 sec; left eye median increase of 0.9 sec, 95% CI from 0.3 to 1.5 sec)(p=0.02
right eye; p=0.004 left eye). The mean Oxford Scheme grade staining decreased significantly during the entire period of the examination
(right eye median decrease of -1.0 grade, 95% CI from -1.0 to -1.0 grade; left eye median decrease of -1.0 grade, 95% CI from -1.0
to -1.0 grade after three months)(p<0.001 both sides). The subjective complaints of the patients measured with the OSDI questionnaire
showed a significant improvement after 3 months’ treatment (median decrease of -13.1 scores, 95% CI from -25.0 to -8.3 scores)(p<0.001).
During the study period, two patients complained of a greasy sensation on their eyelids, but they did not stop the treatment.
No other adverse reactions were reported.
Based on the results of this trial, the
Hungarian health authorities approved the amendment of the LO2A labeling to include the treatment of DES patients suffering from
CCH, and patents were filed in the United States, Israel and Japan for the use of the active component of the drug for treating
A further Phase II study was performed at
Semmelweis University, Budapest, Hungary in 2016. This study explored the safety and efficacy of LO2A in patients with moderate
severity dry eye associated with Sjögren’s where the ocular surface showed Lissamine Green staining causing marked subjective
symptoms using the OSDI questionnaire. Twenty-one patients applied LO2A eye drops to both eyes in a single arm, open label study.
Patients applied 4 drops a day to each eye for 3 months. LIPCOF score, Lissamine Green staining, tear production and OSDI questionnaire
were measured. The study demonstrated a reduction in the LIPCOF score, a decrease in Lissamine Green staining according to
the Oxford scale and mitigation of subjective symptoms of dry eye according to the OSDI questionnaire. However, there was no change
in tear production during the study.
We are evaluating such information and are
considering the potential consequences on our business. In addition, we plan to use the clinical results and approval received
in the Netherlands the treatment of Sjögren’s to assist our Company in the registration of LO2A as a treatment for Sjögren’s
in the Licensed Territories.
Our Clinical Trials
We are currently conducting a multi-center
trial at five different centers in Israel that commenced in August 2016 (the “Multi-Center Trial”). The Multi-Center
Trial is a Phase II randomized, double-blind, placebo-controlled study carried out in parallel groups that is evaluating the safety
and efficacy of LO2A for patients suffering from moderate to severe CCH. The trial completed enrollment of all 62 patients on
March 26, 2018, with the treatment time for each patient being 3 months. The primary efficacy endpoint for this study is the change
from baseline in lissamine green conjunctival staining score at 3 months; secondary endpoints include change from baseline in
lissamine green conjunctival staining score at 1 month, change from baseline in LIPCOF score at 1 and 3 months, change from baseline
in TFBUT at 1 and 3 months and change from baseline in OSDI questionnaire score at 1 and 3 months. Safety endpoints include adverse
events recorded throughout the trial, best-corrected visual acuity, slit lamp biomicroscopy findings, undilated fundoscopy findings
and intraocular pressure measurements. We consulted with ophthalmology consultants from the United States in the preparation of
the protocol for the Multi-Center Trial.
It is envisioned that the clinical study
required for approval in Israel will be of a similar design to the Multi-Center Trial, but appropriately powered to demonstrate
clinical significance according to the treatment effect observed in the current study. We will consult with the Israel Ministry
of Health before a registration study to confirm acceptability of the efficacy endpoints.
The comprehensive cost of the Multi-Center
Trial is estimated at $850,000. As of March 26, 2018, the Multi-Center Trial had completed enrollment of all of the planned 62
patients, with the treatment time for each patient being three months.
On October 26, 2017, Wize Israel announced
the termination of its single center trial (the “Single Center Trial”). The Single Center Trial was a Phase II, randomized,
double-blind, placebo-controlled, pilot study carried out in parallel groups that was intended to evaluate the safety and efficacy
of LO2A for patients suffering from moderate to severe CCH, with Wize Israel having sole access to the trial data. On October 24,
2017, Wize Israel received notice from the contract research organization (“CRO”) that manages and supervises Wize
Israel’s clinical trials, that an inadequate amount of quality information may be derived from the results collected thus
far, given that there is no correlation in the reaction of both eyes to LO2A, in contrast to professional literature and other
trials. In addition, the recruitment rate of patients was less than required and there was a higher than expected dropout rate.
In light of the above, the CRO concluded that the results of the trial would be of no use even if the trial continued until the
end of its term. Based on the CRO’s conclusion, Wize Israel determined to terminate the trial and to save the future costs
that would be incurred in connection with such trial.
In February 2018, we received Institutional
Review Board (IRB) approval for the protocol of our planned Phase IV Study, which is a randomized, double-masked, study of LO2A
versus Alcon’s Systane® Ultra UD, an over-the-counter lubricant eye drop product used to relieve dry and
irritated eyes. The Phase IV Study will take place in Israel and will evaluate the safety and efficacy of LO2A for symptomatic
improvement of DES in 60 adult patients with Sjögren’s. Enrolled patients will be randomized in a 1:1 ratio to one
of two treatment groups, LO2A or Systane® Ultra UD. Drops will be administered topically to the eye over a three
month period. The primary efficacy endpoint for this study is change from baseline in corneal and conjunctival staining score
at 3 months. Secondary efficacy endpoints include change from baseline in corneal and conjunctival staining score at 1 month,
change from baseline in eye dryness score (visual analogue scale) at 1 and 3 months and change from baseline in OSDI questionnaire
score at 1 and 3 months. Safety will be evaluated by collection of adverse event data throughout the study, best-corrected visual
acuity and slit lamp biomicroscopy findings.
This Phase IV Study is designed to support
our clinical approval pathway for LO2A for the treatment of DES in patients with Sjögren’s within certain markets including
the U.S., China, Ukraine and Israel. We enrolled our first patient in the Phase IV Study in the end of March 2018. Data obtained
from this study will be submitted to the Israel Ministry of Health and will be included in the clinical data package submitted
during interactions with the FDA. The study is considered necessary as the existing clinical data in this indication is considered
of insufficient quality for submission to the regulatory agencies mentioned above.
We currently do not have sufficient funds
to complete the Phase IV Study. The completion of such study is contingent upon our ability to raise additional funds.
Research and development expenses for the
year ended December 31, 2017 were approximately $450,000 and for the year ended December 31, 2016 were approximately $240,000.
Raw Materials and Suppliers
We believe that the raw materials that would
be required to manufacture LO2A are widely available from numerous suppliers and are generally considered to be generic industrial
There can be no assurance that LO2A can
be manufactured in sufficient commercial quantities, in compliance with regulatory requirements and at an acceptable cost. We and
our contract manufacturers are, and will be, subject to extensive governmental regulation in connection with LO2A. We and our manufacturer
must ensure that all of the processes, methods and equipment are compliant with both cGMP, and current Good Laboratory Practices
for drugs on an ongoing basis, as mandated by the applicable regulatory authorities, and conduct extensive audits of vendors, contract
laboratories and suppliers. We have entered into agreements with a manufacturer in Germany relating to the manufacturing of LO2A.
We have completed the production of LO2A for purposes of our ongoing Phase II clinical trial and expect to begin production for
commercial use only after obtaining the requisite regulatory approvals in Israel and Ukraine to market LO2A and receive orders
from the distributors (for more information, see “—Marketing, Sales and Distribution” below).
Marketing, Sales and Distribution
We plan to engage local or multinational
distributors to handle the distribution of LO2A. In particular, we intend to enter into agreements with pharmaceutical companies
with relevant marketing capabilities in the field of pharmaceuticals in order to have them distribute and sell LO2A in the Licensed
Territories. To date, we have entered into exclusive distribution agreements in Israel to market LO2A for the treatment of DES,
and in Ukraine for the treatment of DES and CCH. The registration process in certain countries, including the United States, requires
us to undertake additional clinical trials, in addition to the Phase II clinical trials that we are currently conducting. In August,
2015, LO2A received the approval of the Israel Ministry of Health for use in Israel as a medical preparation for the treatment
of DES, under the brand name “Eyecon®”. Registration of LO2A was submitted in Ukraine by the Ukrainian
distributor for use in Ukraine as a medical preparation for the treatment of DES and CCH, under the brand name “Conheal®”.
The registration in Ukraine is conducted by the Ukrainian distributor and he informed us that it is expected to be completed in
the second half of 2018. In July 2017, we received our first order from the distributor in Israel, for an immaterial amount.
On November 3, 2017, Wize Israel entered
into a framework agreement with a Chinese pharmaceutical company (the “Chinese Distributor”), whereby, subject to the
negotiation and execution of a detailed distribution agreement and obtaining necessary regulatory approvals in China, the Chinese
Distributor will act as exclusive distributor in China of LO2A. The framework agreement includes, among other things, minimum purchase
obligations of the Chinese Distributor, which Wize Israel estimated to range, over the five-year period of the contemplated agreement,
between $22.5 million to $39 million. As of the date hereof, no detailed distribution agreement has been entered into with the
Chinese Distributor and the regulatory process has not been completed and it is not possible at this stage to determine when these
conditions will be completed, if ever, and, even if completed, the final terms of such detailed distribution agreement and the
expected revenues therefrom. The Chinese Distributor plans to import LO2A from one of the existing European countries, most likely
Hungary, and thus the indications shall include DES and any additional indication already approved in the specific European country.
If such indications are imported from Hungary, the indications would include DES and CCH. Clinical trials in China may be required
by the China Food and Drug Administration (“CFDA”) as part of the regulatory requirements for approving LO2A in China.
At this stage it is not certain whether such clinical trials will be required.
We intend to engage pharmaceutical companies
or distributors around the world with relevant marketing capabilities in the pharmaceutical field, in order for such pharmaceutical
companies to sell LO2A, with us prioritizing those countries where we may expedite the registration process of LO2A based on existing
knowledge and studies previously conducted on LO2A, without requiring additional studies. In this respect, we have been studying
the possibility of marketing LO2A for DES treatment only in the United States, but have not made any determinations regarding the
best route that can be used to obtain FDA approval to market LO2A. Currently, we intend to approach the FDA as part of our preliminary
request procedure (Pre-IND) and discuss possible alternatives for approving LO2A for treating DES in the United States. However,
as this FDA process is both time consuming and costly, we do not intend to approach the FDA on a Pre-IND basis until we are able
to secure additional funding.
The pharmaceutical industry is characterized
by rapidly evolving technology, intense competition and a highly risky, costly and lengthy research and development process. Adequate
protection of intellectual property, successful product development, adequate funding and retention of skilled, experienced and
professional personnel are among the many factors critical to success in the pharmaceutical industry. We operate in markets
featuring competition between competing manufacturers in the field of DES treatment, while, to our knowledge, no therapy is currently
approved specifically for Sjögren’s or CCH.
The global DES market features three particularly
dominant companies, which are responsible for an estimated 82% of all revenues: Novartis/Alcon (through its Celluvisc®,
Hyalein®, Vismed® and Systane® drugs); Allergan (Restasis®, Refresh®)
and Santen. In July 2016, the FDA approved an additional medicine, Xiidra®, produced by Shire Plc, for the treatment
of DES, and sales began in August 2016.
To date, no therapeutic agent has received
approval specifically for Sjögren’s. Drugs that are used for the symptomatic relief of ocular signs and symptoms associated
with Sjögren’s include cholinergic agonists e.g. Salagen (pilocarpine) and Evoxac (cevilemine) and the immunomodulatory
agent Restasis (cyclosporine). Systemic Immunomodulary treatments, usually for extra-glandular disease, which may be used
include hydroxychloroquine (mild inflammatory symptoms of joints, muscles and skin), corticosteroids (rare but serious symptoms:
vasculitic rash, interstitial lung disease, interstitial nephritis, glomerulonephritis), immunosuppressive agents e.g. methotrexate,
azathioprine, cyclophosphamide (used to treat serious internal organ manifestations) and biologic agents e.g. rituximab. Corticosteroids
and immunosuppressants lead to broad, non-selective immunosuppression often associated with significant adverse events.
The pipeline of drugs in development for
the indication of Sjögren’s is relatively small with only one product in Phase III, Orencia, being developed by
Bristol-Myers Squibb. There are a number of drugs in Phase I or II stages of development including AMG/MEDI5872 developed
by Amgen, BIIB063 developed by Biogen, CFZ533 and VAY736 developed by Novartis, GSK618960 developed by GSK, LY3090106 developed
by Eli Lilly, MEDI4920 developed by MedImmune, RG7625 developed by Roche, RSLV developed by Resolve Therapeutics and Actemra
developed by the University Hospital of Strasbourg. In addition, there is an ongoing Phase II combination study combining
Benlysta and Rituxan.
We believe that LO2A has a number of advantages
over competing products in the DES and Sjögren’s markets, including LO2A lacking preservatives, its ability to be used
with any contact lenses, its anti-irritant properties and its non-Newtonian viscosity profile. On the other hand, other drugs on
the market, including new drugs under development, may all be competitive to LO2A. In fact, some of these drugs are well
established and accepted among patients and physicians in their respective markets, can be efficiently produced and marketed, and
are relatively safe. Moreover, other companies of various sizes engage in activities similar to ours. Most, if not
all, of our competitors have substantially greater financial and other resources available to them. Competitors include companies
with marketed products and/or an advanced research and development pipeline.
Our success depends in part on our ability
(directly or through Resdevco) to obtain and maintain proprietary protection for LO2A and its underlying technology and know-how,
and to operate without infringing the proprietary rights of others and to prevent others from infringing such proprietary rights.
The LO2A composition and use thereof for
treating or alleviating DES was covered by US Patent No. 5,106,615, which has expired. Accordingly, we are currently focusing our
marketing and commercial efforts with respect to CCH and Sjögren’s rather than DES, as more fully described elsewhere
in this Annual Report. The use of LO2A for treating or alleviating CCH under US Patent No. 8,912,166 has been granted to us under
the LO2A License Agreement.
The use of LO2A for treating or alleviating
CCH is protected by the patent family of International Patent Application Publ. No. WO2012150583, filed on April 5, 2012, assigned
to Resdevco, entitled EYE DROPS FOR TREATMENT OF CONJUNCTIVOCHALASIS. Corresponding members include US Patent No. 8,912,166, Israeli
Patent No. 212725, Japanese Patent No. 5957517 and pending European Pat. Appl. 2704747. Granted patents and patents to issue of
this patent family will expire, without extension, in 2032.
The use of LO2A for treating or alleviating
irritation of the eye caused non-infectious diseases, such as Sjögren’s, is covered by Provisional Patent Application
No. 62/467139, filed on March 5, 2017, assigned to Resdevco, entitled EYE DROPS FOR TREATMENT OF IRRITATION NOT DUE TO INFECTION.
Patents to issue based on this provisional application will expire, without extension, in 2038.
Pursuant to the LO2A License Agreement,
Resdevco has contractually agreed to be responsible for the payment of all relevant fees associated with the maintenance of its
intellectual property rights. The patent positions of biopharmaceutical companies, such as Resdevco and us, are generally uncertain
and involve complex legal and factual questions. Resdevco’s ability to maintain and solidify its proprietary position for
LO2A will depend on its success in obtaining effective claims and enforcing those claims once granted. There is no certainty that
any of Resdevco’s pending patent applications or those pending patent applications that it licenses will result in the issuance
of any patents or that we will obtain rights to any further patents or patent applications. Any issued patents and those that
may issue in the future may be challenged, narrowed, circumvented or found to be invalid or unenforceable, which could limit our
ability to stop competitors from marketing related products or the length of term of patent protection that we may have for LO2A
under the LO2A License Agreement. We cannot be certain that Resdevco was the first to invent the inventions claimed in its owned
or licensed patents or pending patent applications. In addition, our competitors may independently develop similar technologies
or duplicate any technology developed by Resdevco, and the rights granted under any issued patents may not provide Resdevco or
us with any meaningful competitive advantages against these competitors. Please see under Item 1A - “RISK FACTORS –
Risks Related to our Intellectual Property,” beginning on page 47 of this Annual Report.
We and our manufacturers, distributors and
other service providers are subject to various environmental, health and safety laws and regulations, including those governing
air emissions, water and wastewater discharges, noise emissions, the use, management and disposal of hazardous, radioactive and
biological materials and wastes and the cleanup of contaminated sites. We believe that our business, including those of our service
providers, are being operated in compliance in all material respects with applicable environmental and health and safety laws and
regulations. Based on information currently available to us, we do not expect environmental costs and contingencies to have a material
adverse effect on our business. However, significant expenditures may be imposed on those third party service providers should
they be required to comply with new or more stringent environmental or health and safety laws, regulations or requirements, which
may in turn adversely affect us.
We operate in a highly controlled regulatory
environment. Stringent regulations establish requirements relating to analytical, toxicological and clinical standards and protocols
in respect of the testing of pharmaceuticals. Regulations also cover research, development, manufacturing and reporting procedures,
both pre- and post-approval. In many markets, especially in Europe, marketing and pricing strategies are subject to national legislation
or administrative practices that include requirements to demonstrate not only the quality, safety and efficacy of a new product,
but also its cost-effectiveness relating to other treatment options. Failure to comply with regulations can result in stringent
sanctions, including product recalls, withdrawal of approvals, seizure of products and criminal prosecution.
Before obtaining regulatory approvals for
the commercial sale of LO2A or any of our future product candidates, we must demonstrate through clinical trials that any of our
product candidates are safe and effective. Historically, the results from preclinical studies and early clinical trials often have
not accurately predicted results of later clinical trials. In addition, a number of pharmaceutical products have shown promising
results in clinical trials but subsequently failed to establish sufficient safety and efficacy results to obtain necessary regulatory
approvals. We have incurred and will continue to incur substantial expense for, and devote a significant amount of time to, clinical
trials. Many factors can delay the commencement and rate of completion of clinical trials, including the inability to recruit patients
at the expected rate, the inability to follow patients adequately after treatment, the failure to manufacture sufficient quantities
of materials used for clinical trials, and the emergence of unforeseen safety issues and governmental and regulatory delays. If
a product candidate fails to demonstrate safety and efficacy in clinical trials, this failure may delay development of other product
candidates and hinder our ability to conduct related clinical trials. Additionally, as a result of these failures, we may also
be unable to obtain additional financing.
Governmental authorities in all major markets
require that a new pharmaceutical product be approved before it is marketed, and have established high standards for technical
appraisal, which can result in an expensive and lengthy approval process. The time to obtain approval varies by country and some
products are never approved. The lengthy process of conducting clinical trials, seeking approval and the subsequent compliance
with applicable statutes and regulations, if approval is obtained, are very costly and require the expenditure of substantial resources.
of the regulatory processes in countries where we are seeking or will seek regulatory approval
In the United States, the Public Health
Services Act and the Federal Food, Drug, and Cosmetic Act, as amended, and the regulations promulgated thereunder, and other federal
and state statutes and regulations govern, among other things, the quality, safety and effectiveness standards for any of our product
candidates and the raw materials and components used in the production of, testing, manufacture, labeling, storage, record keeping,
approval, advertising and promotion of our products on a product-by-product basis.
Before the clinical studies, the FDA requires
from the applicants to complete extensive preclinical laboratory tests, drug chemistry, animal (in vivo), formulation, stability
and other studies.
Certain preclinical tests must be conducted
in compliance with good laboratory practice (GLP) regulations. Non-compliance with GLP standard can, in some cases, lead
to invalidation of the studies, requiring them to be replicated. After laboratory analysis and preclinical testing, a sponsor
files an Investigational New Drug (“IND”) application, with the FDA to begin human testing.
The results of the preclinical studies,
together with manufacturing information and analytical data, are submitted to the FDA as part of an IND application. The IND automatically
becomes effective 30 days after receipt by the FDA, unless the FDA, within the 30-day time period, raises concerns or questions
about the conduct of the clinical trial, including concerns that human research subjects will be exposed to unreasonable health
risks. In such a case, the IND sponsor and the FDA must resolve any outstanding concerns before the clinical trial can begin. Submission
of an IND may result in the FDA not allowing the clinical trials to commence or not allowing the clinical trials to commence on
the terms originally specified in the IND. A separate submission to an existing IND must also be made for each successive clinical
trial conducted during drug development, and the FDA must grant permission, either explicitly or implicitly by not objecting, before
each clinical trial can begin.
Typically, a manufacturer conducts a three-phase
human clinical testing program which itself is subject to numerous laws and regulatory requirements, including adequate monitoring,
reporting, record keeping and informed consent.
Clinical trials involve the administration
of the investigational drug to human subjects under the supervision of qualified investigators. Clinical trials are conducted under
protocols detailing, among other things, the objectives of the clinical trial, the parameters to be used in monitoring safety and
the effectiveness criteria to be used. Each protocol must be submitted to the FDA as part of the IND. An independent institutional
review board (“IRB”), for each medical center proposing to conduct a clinical trial must also review and approve a
plan for any clinical trial before it can begin at that center and the IRB must monitor the clinical trial until it is completed.
The FDA, the IRB, or the sponsor may suspend or discontinue a clinical trial at any time on various grounds. Clinical testing also
must satisfy extensive Good Clinical Practice (“GCP”), requirements, including the requirements for informed consent.
All clinical research performed in the United
States in support of a new drug application (“NDA”) must be authorized in advance by the FDA under the IND regulations
and procedures described above. However, a sponsor who wishes to conduct a clinical trial outside the United States may, but need
not, obtain FDA authorization to conduct the clinical trial under an IND. If a foreign clinical trial is not conducted under an
IND, the sponsor may submit data from the clinical trial to FDA in support of an NDA so long as the clinical trial is conducted
in compliance with an international guideline for the ethical conduct of clinical research known as the Declaration of Helsinki
and/or the laws and regulations of the country or countries in which the clinical trial is performed, whichever provides the greater
protection to the participants in the clinical trial.
In Phase I, small clinical trials are conducted
to determine the safety and proper dose ranges of any of our product candidates. In Phase II, clinical trials are conducted
to assess safety and gain preliminary evidence of the efficacy of any of our product candidates. In Phase III, clinical trials
are conducted to provide sufficient data for the statistically valid evidence of safety and efficacy and these studies include
a large number of participants. The time and expense required for us to perform this clinical testing can vary and is substantial.
We cannot be certain that we will successfully complete Phase I, Phase II or Phase III testing of any of our product candidates
within any specific time period, if at all. Furthermore, the FDA, the IRB responsible for approving and monitoring the clinical
trials at a given site, the Data Safety Monitoring Board, where one is used, or we may suspend the clinical trials at any time
on various grounds, including a finding that subjects or patients are exposed to unacceptable health risk.
If the clinical data from these clinical
trials (Phases I, II and III) is deemed to support the safety and effectiveness of the candidate product for its intended use,
then we may proceed to seek to file with the FDA an NDA seeking approval to market a new drug for one or more specified intended
uses. We cannot ascertain whether the clinical data will support and justify filing an NDA. Nevertheless, if and when we are able
to ascertain that the clinical data supports and justifies filing an NDA, we intend to make such appropriate filings.
The purpose of an NDA is to provide the
FDA with sufficient information so that it can assess whether it ought to approve the candidate product for marketing for specific
intended uses. The NDA normally contains, among other things, sections describing the chemistry, manufacturing, and controls, non-clinical
pharmacology and toxicology, human pharmacokinetics and bioavailability, microbiology, the results of the clinical trials, and
the proposed labeling which contains, among other things, the intended uses of the candidate product.
We cannot take any action to market any
new drug or biologic product in the United States until our appropriate marketing application has been approved by the FDA. The
FDA has substantial discretion over the approval process and may disagree with our interpretation of the data submitted.
The process may be significantly extended by requests for additional information or clarification regarding information already
provided. As part of this review, the FDA may refer the application to an appropriate advisory committee, typically a panel
of clinicians. Satisfaction of these and other regulatory requirements typically takes several years, and the actual time
required may vary substantially based upon the type, complexity and novelty of the product. Government regulation may delay
or prevent marketing of potential products for a considerable period of time and impose costly procedures on our activities. We
cannot be certain that the FDA or other regulatory agencies will approve any of our products on a timely basis, if at all. Success
in early stage clinical trials does not assure success in later-stage clinical trials. Even if a product receives regulatory
approval, the approval may be significantly limited to specific indications or uses and these limitations may adversely affect
the commercial viability of the product. Delays in obtaining, or failures to obtain regulatory approvals, would have a material
adverse effect on our business.
We may also seek approval under programs
designed to accelerate the FDA’s review and approval of NDAs. For instance, a sponsor may seek FDA designation of a drug
candidate as a “fast track product.” Fast track products are those products intended for the treatment of a serious
or life-threatening disease or condition and which demonstrate the potential to address unmet medical needs for such disease or
condition. If fast track designation is obtained, the FDA may initiate review of sections of an NDA before the application is complete.
This “rolling review” is available if the applicant provides and the FDA approves a schedule for submission to the
FDA of the remaining information. In some cases, a fast track product may be approved on the basis of either a surrogate endpoint
that is reasonably likely to predict clinical benefit, or on a clinical endpoint that can be measured earlier than irreversible
morbidity or mortality, that is reasonably likely to predict an effect on irreversible morbidity or mortality or other clinical
benefit, taking into account the severity, rarity, or prevalence of the condition and the availability or lack of alternative treatments.
Approvals of this kind, referred to as accelerated approvals, typically include requirements for appropriate post-approval Phase
IV clinical trials to validate the surrogate endpoint or otherwise confirm the effect of the clinical endpoint.
In addition, the Food and Drug Administration
Safety and Innovation Act, which was enacted and signed into law in 2012, established a new category of drugs referred to as “breakthrough
therapies” that may be subject to accelerated approval. A sponsor may seek FDA designation of a drug candidate as a “breakthrough
therapy” if the drug is intended, alone or in combination with one or more other drugs, to treat a serious or life-threatening
disease or condition and preliminary clinical evidence indicates that the drug may demonstrate substantial improvement over existing
therapies on one or more clinically significant endpoints, such as substantial treatment effects observed early in clinical development.
Drug candidates may also be eligible for “priority review,” or review within a six-month timeframe from the date a
complete NDA is accepted for filing, if a sponsor shows that its drug candidate provides a significant improvement compared to
marketed drugs. Fast track designation, accelerated approval, breakthrough therapy designation and priority review do not change
the standards for approval, but may expedite the development or approval process. When appropriate, we intend to seek fast track
designation, accelerated approval, breakthrough therapy designation and priority review, as applicable for our drug candidates.
We cannot predict whether any of our drug candidates will obtain such designations or approvals, or the ultimate impact, if any,
of such designations or approvals on the timing or likelihood of FDA approval of any of its proposed drugs.
Even after we obtain FDA approval, we may
be required to conduct further clinical trials (i.e., Phase IV trials) and provide additional data on safety and effectiveness.
We are also required to gain separate approval for the use of an approved product as a treatment for indications other than
those initially approved. Before approving an application, the FDA will inspect the facility or the facilities at which the
finished drug product, and sometimes the active drug ingredient, is manufactured, and will not approve the drug unless cGMP compliance
is satisfactory. The FDA may also inspect the sites at which the clinical trials were conducted to assess their compliance, and
will not approve the drug unless compliance with GCP requirements is satisfactory.
If, as a result of these inspections, the
FDA determines that our facilities do not comply with applicable FDA regulations and conditions of product approval, the FDA may
seek civil, criminal or administrative sanctions and/or remedies against us including the suspension of our manufacturing operations.
Drugs may be marketed only for the FDA approved
indications and in accordance with the provisions of the approved labeling. Further, if there are any modifications to the drug,
including changes in indications, labeling, or manufacturing processes or facilities, the applicant may be required to submit and
obtain FDA approval of a new NDA or NDA supplement, which may require us to develop additional data or conduct additional preclinical
studies and clinical trials.
We have currently received no approvals
to market our products from the FDA or other foreign regulators, besides Israel and the countries where LO2A is already marketed
Following approval of a new product, a pharmaceutical
company generally must engage in numerous specific monitoring and recordkeeping activities and continue to submit periodic and
other reports to the applicable regulatory agencies, including any cases of adverse events and appropriate quality control records.
Modifications or enhancements to the products or labeling or changes of site of manufacture are often subject to the approval of
the FDA and other regulators, which may or may not be received or may result in a lengthy review process.
Prescription drug advertising is subject
to federal, state and foreign regulations. In the United States, the FDA regulates prescription drug promotion, including direct-to-consumer
advertising. Prescription drug promotional materials must be submitted to the FDA in conjunction with their first use. Any distribution
of prescription drug products and pharmaceutical samples must comply with the U.S. Prescription Drug Marketing Act, a part of the
U.S. Federal Food, Drug, and Cosmetic Act.
In the United States, once a product is
approved, its manufacture is subject to comprehensive and continuing regulation by the FDA. The FDA regulations require that products
be manufactured in specific approved facilities and in accordance with current good manufacturing practices, or cGMPs, and NDA
holders must list their products and register their manufacturing establishments with the FDA. These regulations also impose certain
organizational, procedural and documentation requirements with respect to manufacturing and quality assurance activities. NDA holders
using contract manufacturers, laboratories or packagers are responsible for the selection and monitoring of qualified firms, and,
in certain circumstances, qualified suppliers to these firms. These firms and, where applicable, their suppliers are subject to
inspections by the FDA at any time, and the discovery of violative conditions, including failure to conform to cGMPs, could result
in enforcement actions that interrupt the operation of any such facilities or the ability to distribute products manufactured,
processed or tested by them.
Healthcare Laws and Regulations
We are also subject to various federal,
state and international laws pertaining to health care “fraud and abuse,” including anti-kickback laws and false claims
laws. The federal Anti-kickback law, which governs federal healthcare programs (e.g., Medicare, Medicaid), makes it illegal
to solicit, offer, receive or pay any remuneration in exchange for, or to induce, the referral of business, including the purchase
or prescription of a particular drug. Many states have similar laws that are not restricted to federal healthcare programs.
Federal and state false claims laws prohibit anyone from knowingly and willingly presenting, or causing to be presented for
payment to third party payors (including Medicare and Medicaid), claims for reimbursement, including claims for the sale of drugs
or services, that are false or fraudulent, claims for items or services not provided as claimed, or claims for medically unnecessary
items or services.
If the government or other relevant party
were to allege that we violated these laws there could be a material adverse effect on our stock price. Even an unsuccessful
challenge could cause adverse publicity and be costly to respond to, which could have a materially adverse effect on our business,
results of operations and financial condition. A finding of liability under these laws can have significant adverse financial
implications for us and can result in payment of large penalties and possible exclusion from federal healthcare programs. We
will consult counsel concerning the potential application of these and other laws to our business and our sales, marketing and
other activities and will make good faith efforts to comply with them. However, given their broad reach and the increasing
attention given by law enforcement authorities, we cannot assure you that some of our activities will not be challenged or deemed
to violate some of these laws.
European Economic Area
Although we are not currently seeking regulatory
approval in the European Union (“EU”), we may do so in the future. As such, a summary of the EU regulatory processes
A medicinal product may only be placed on
the market in the European Economic Area (the “EEA”), composed of the 28 EU member states, plus Norway, Iceland and
Lichtenstein, when a marketing authorization has been issued by the competent authority of a member state pursuant to Directive
2001/83/EC (as recently amended by Directive 2004/27/EC), or an authorization has been granted under the centralized procedure
in accordance with Regulation (EC) No. 726/2004 or its predecessor, Regulation 2309/93. There are essentially three community procedures
created under prevailing European pharmaceutical legislation that, if successfully completed, allow an applicant to place a medicinal
product on the market in the EEA.
Regulation 726/2004/EC now governs the centralized
procedure when a marketing authorization is granted by the European Commission, acting in its capacity as the European Licensing
Authority on the advice of the EMA. That authorization is valid throughout the entire community and directly or (as to Norway,
Iceland and Liechtenstein) indirectly allows the applicant to place the product on the market in all member states of the EEA.
The EMA is the administrative body responsible for coordinating the existing scientific resources available in the member states
for evaluation, supervision and pharmacovigilance of medicinal products. Certain medicinal products, as described in the Annex
to Regulation 726/2004, must be authorized centrally. These are products that are developed by means of a biotechnological process
in accordance with Paragraph 1 to the Annex to the Regulation. Medicinal products for human use containing a new active substance
for which the therapeutic indication is the treatment of acquired immune deficiency syndrome, or AIDS, cancer, neurodegenerative
disorder or diabetes must also be authorized centrally. Starting on May 20, 2008, the mandatory centralized procedure was extended
to autoimmune diseases and other immune dysfunctions and viral diseases. Finally, all medicinal products that are designated as
orphan medicinal products pursuant to Regulation 141/2000 must be authorized under the centralized procedure. An applicant may
also opt for assessment through the centralized procedure if it can show that the medicinal product constitutes a significant therapeutic,
scientific or technical innovation or that the granting of authorization centrally is in the interests of patients at the community
level. For each application submitted to the EMA for scientific assessment, the EMA is required to ensure that the opinion of the
Committee for Medicinal Products for Human Use (“CHMP”), is given within 210 days after receipt of a valid application.
This 210 days period does not include the time that the applicant to answer any questions raised during the application procedure,
the so-called ‘clock stop’ period. If the opinion is positive, the EMA is required to send the opinion to the European
Commission, which is responsible for preparing the draft decision granting a marketing authorization. This draft decision may differ
from the CHMP opinion, stating reasons for diverging for the CHMP opinion. The draft decision is sent to the applicant and the
member states, after which the European Commission takes a final decision. If the initial opinion of the CHMP is negative, the
applicant is afforded an opportunity to seek a re-examination of the opinion. The CHMP is required to re-examine its opinion within
60 days following receipt of the request by the applicant. All CHMP refusals and the reasons for refusal are made public on the
EMA website. Without a centralized marketing authorization it is prohibited to place a medicinal product that must be authorized
centrally on the market in the EU.
This procedure is available for medicinal
products that do not fall within the scope of mandatory centralized authorization and are intended for use in only one EU member
state. Specific procedures and timelines differ between member states, but the duration of the procedure is generally 210 days
and based on a risk/efficacy assessment by the competent authority of the member state concerned, followed by determination of
Summary of Product Characteristics (“SmPC”) package leaflet and label text/layout and subsequently grant of the marketing
authorization. Marketing authorizations granted on this basis are not mutually recognized by other member states.
The majority of medicines available in the
EU were authorized at national level, either because they were authorized before EMA’s creation or they were not in the scope
of the centralized procedure. Each EU Member State has its own national authorization procedures. If a company wishes to request
marketing authorization in several EU Member States for a medicine that is outside the scope of the centralized procedure, it may
use one of the following routes:
||the mutual-recognition procedure, whereby a marketing authorization granted in one Member State can be recognized in other EU countries; or|
||the decentralized procedure, whereby a medicine that has not yet been authorized in the EU can be simultaneously authorized in several EU Member States.|
Mutual Recognition and Decentralized Procedures
With the exception of products that are
authorized centrally, the competent authorities of the member states are responsible for granting marketing authorizations for
medicinal products placed on their national markets. If the applicant for a marketing authorization intends to market the same
medicinal product in more than one member state, the applicant may seek an authorization progressively in the community under the
mutual recognition or decentralized procedure. Mutual recognition is used if the medicinal product has already been authorized
in a member state. In this case, the holder of this marketing authorization requests the member state where the authorization has
been granted to act as reference member state by preparing an updated assessment report that is then used to facilitate mutual
recognition of the existing authorization in the other member states in which approval is sought (the so-called concerned member
state(s)). The reference member state must prepare an updated assessment report within 90 days of receipt of a valid application.
This report together with the approved SmPC (which sets out the conditions of use of the product), and a labeling and package leaflet
are sent to the concerned member states for their consideration. The concerned member states are required to approve the assessment
report, the SmPC and the labeling and package leaflet within 90 days of receipt of these documents. The total procedural time is
The decentralized procedure is used in cases
where the medicinal product has not received a marketing authorization in the EU at the time of application. The applicant requests
a member state of its choice to act as reference member state to prepare an assessment report that is then used to facilitate agreement
with the concerned member states and the grant of a national marketing authorization in all of these member states. In this procedure,
the reference member state must prepare, for consideration by the concerned member states, the draft assessment report, a draft
SmPC and a draft of the labeling and package leaflet within 120 days after receipt of a valid application. As in the case of mutual
recognition, the concerned member states are required to approve these documents within 90 days of their receipt.
For both mutual recognition and decentralized
procedures, if a concerned member state objects to the grant of a marketing authorization on the grounds of a potential serious
risk to public health, it may raise a reasoned objection with the reference member state. The points of disagreement are in the
first instance referred to the Co-ordination Group on Mutual Recognition and Decentralized Procedures (“CMD”), to reach
an agreement within 60 days of the communication of the points of disagreement. If member states fail to reach an agreement, then
the matter is referred to the EMA and CHMP for arbitration. The CHMP is required to deliver a reasoned opinion within 60 days of
the date on which the matter is referred. The scientific opinion adopted by the CHMP forms the basis for a binding European Commission
Irrespective of whether the medicinal product
is assessed centrally, de-centrally or through a process of mutual recognition, the medicinal product must be manufactured in accordance
with the principles of good manufacturing practice as set out in Directive 2003/94/EC and Volume 4 of the rules governing medicinal
products in the European community. Moreover, community law requires the clinical results in support of clinical safety and efficacy
based upon clinical trials conducted in the European community to be in compliance with the requirements of Directive 2001/20/EC,
which implements good clinical practice in the conduct of clinical trials on medicinal products for human use. Clinical trials
conducted outside the European community and used to support applications for marketing within the EU must have been conducted
in a way consistent with the principles set out in Directive 2001/20/EC. The conduct of a clinical trial in the EU requires, pursuant
to Directive 2001/20/EC, authorization by the relevant national competent authority where a trial takes place, and an ethics committee
to have issued a favorable opinion in relation to the arrangements for the trial. It also requires that the sponsor of the trial,
or a person authorized to act on his behalf in relation to the trial, be established in the community.
There are various types of applications
for marketing authorizations:
A full application is one that is made under
any of the community procedures described above and “stands alone” in the sense that it contains all of the particulars
and information required by Article 8(3) of Directive 2001/83 (as amended) to allow the competent authority to assess the quality,
safety and efficacy of the product and in particular the balance between benefit and risk. Article 8(3)(l) in particular refers
to the need to present the results of the applicant’s research on (i) pharmaceutical (physical-chemical, biological or microbiological)
tests, (ii) preclinical (toxicological and pharmacological) studies and (iii) clinical trials in humans. The nature of these tests,
studies and trials is explained in more detail in Annex I to Directive 2001/83/EC. Full applications would be required for products
containing new active substances not previously approved by the competent authority, but may also be made for other products.
Article 10 of Directive 2001/83/EC contains
exemptions from the requirement that the applicant provide the results of its own preclinical and clinical research. There are
three regulatory routes for an applicant to seek an exemption from providing such results, namely (i) cross-referral to an innovator’s
results without consent of the innovator, (ii) well established use according to published literature and (iii) consent to refer
to an existing dossier of research results filed by a previous applicant.
Cross-referral to Innovator’s
Articles 10(1) and 10(2)(b) of Directive
2001/83/EC provide the legal basis for an applicant to seek a marketing authorization on the basis that its product is a generic
medicinal product (a copy) of a reference medicinal product that has already been authorized, in accordance with community provisions.
A reference product is, in principle, an original product granted an authorization on the basis of a full dossier of particulars
and information. This is the main exemption used by generic manufacturers for obtaining a marketing authorization for a copy product.
The generic applicant is not required to provide the results of preclinical studies and of clinical trials if its product meets
the definition of a generic medicinal product and the applicable regulatory results protection period for the results submitted
by the innovator has expired. A generic medicinal product is defined as a medicinal product:
||having the same qualitative and quantitative composition in active substance as the reference medicinal product;|
||having the same pharmaceutical form as the reference medicinal product; and|
||whose bioequivalence with the reference medicinal product has been demonstrated by appropriate bioavailability studies.|
Applications in respect of a generic medicinal
product cannot be made before the expiry of the protection period. Where the reference product was granted a national marketing
authorization pursuant to an application made before October 30, 2005, the protection period is either six years or 10 years, depending
upon the election of the particular member state concerned. Where the reference product was granted a marketing authorization centrally,
pursuant to an application made before November 20, 2005, the protection period is 10 years. For applications made after these
dates, Regulation 726/2004 and amendments to Directive 2001/83/EC provide for a harmonized protection period regardless of the
approval route utilized. The harmonized protection period is in total 10 years, including eight years of research data protection
and two years of marketing protection. The effect is that the originator’s results can be the subject of a cross-referral
application after eight years, but any resulting authorization cannot be exploited for a further two years. The rationale of this
procedure is not that the competent authority does not have before it relevant tests and trials upon which to assess the efficacy
and safety of the generic product, but that the relevant particulars can, if the research data protection period has expired, be
found on the originator’s file and used for assessment of the generic medicinal product. The 10-year protection period can
be extended to 11 years where, in the first eight years post-authorization, the holder of the authorization obtains approval for
a new indication assessed as offering a significant clinical benefit in comparison with existing products.
If the copy product does not meet the definition
of a generic medicinal product or if certain types of changes occur in the active substance(s) or in the therapeutic indications,
strength, pharmaceutical form or route of administration in relation to the reference medicinal product, Article 10(3) of Directive
2001/83/EC provides that the results of the appropriate preclinical studies or clinical trials must be provided by the applicant.
Well-established Medicinal Use
Under Article 10a of Directive 2001/83/EC,
an applicant may, in substitution for the results of its own preclinical and clinical research, present detailed references to
published literature demonstrating that the active substance(s) of a product have a well-established medicinal use within the community
with recognized efficacy and an acceptable level of safety. The applicant is entitled to refer to a variety of different types
of literature, including reports of clinical trials with the same active substance(s) and epidemiological studies that indicate
that the constituent or constituents of the product have an acceptable safety/efficacy profile for a particular indication. However,
use of the published literature exemption is restricted by stating that in no circumstances will constituents be treated as having
a well-established use if they have been used for less than 10 years from the first systematic and documented use of the substance
as a medicinal product in the EU. Even after 10 years’ systematic use, the threshold for well-established medicinal use might
not be met. European pharmaceutical law requires the competent authorities to consider among other factors the period over which
a substance has been used, the amount of patient use of the substance, the degree of scientific interest in the use of the substance
(as reflected in the scientific literature) and the coherence (consistency) of all the scientific assessments made in the literature.
For this reason, different substances may reach the threshold for well-established use after different periods, but the minimum
period is 10 years. If the applicant seeks approval of an entirely new therapeutic use compared with that to which the published
literature refers, additional preclinical and/or clinical results would have to be provided.
Consent to refer to an existing dossier
Under Article 10c of Directive 2001/83/EC,
following the grant of a marketing authorization the holder of such authorization may consent to a competent authority utilizing
the pharmaceutical, preclinical and clinical documentation that it submitted to obtain approval for a medicinal product to assess
a subsequent application relating to a medicinal product possessing the same qualitative and quantitative composition with respect
to the active substances and the same pharmaceutical form.
Law Relating to Pediatric Research
Regulation (EC) 1901/2006 (as amended by
Regulation (EC) 1902/2006) was adopted on December 12, 2006. This Regulation governs the development of medicinal products for
human use in order to meet the specific therapeutic needs of the pediatric population. It requires any application for marketing
authorization made after July 26, 2008 in respect of a product not authorized in the European Community on January 26, 2007 (the
time the Regulation entered into force), to include the results of all studies performed and details of all information collected
in compliance with a pediatric investigation plan agreed by the Pediatric Committee of the EMA, unless the product is subject to
an agreed waiver or deferral or unless the product is excluded from the scope of Regulation 1902/2006 (generics, hybrid medicinal
products, biosimilars, homeopathic and traditional (herbal) medicinal products and medicinal products containing one or more active
substances of well-established medicinal use). Waivers can be granted in certain circumstances where pediatric studies are not
required or desirable. Deferrals can be granted in certain circumstances where the initiation or completion of pediatric studies
should be deferred until appropriate studies in adults have been performed. Moreover, this regulation imposes the same obligation
from January 26, 2009 on an applicant seeking approval of a new indication, pharmaceutical form or route of administration for
a product already authorized and still protected by a supplementary protection certificate granted under Regulation EC 469/2009
and its precursor (EEC) 1768/92 or by a patent that qualifies for the granting of such a supplementary protection certificate.
The pediatric Regulation 1901/2006 also provides, subject to certain conditions, a reward for performing such pediatric studies,
regardless of whether the pediatric results provided resulted in the grant of a pediatric indication. This reward comes in the
form of an extension of six months to the supplementary protection certificate granted in respect of the product, unless the product
is subject to orphan drug designation, in which case the 10-year market exclusivity period for such orphan products is extended
to 12 years. If any of the non-centralized procedures for marketing authorization have been used, the six-month extension of the
supplementary protection certificate is only granted if the medicinal product is authorized in all member states.
In the pre-authorization phase the applicant
must provide a detailed pharmacovigilance plan that it intends to implement post-authorization. An authorization to market a medicinal
product in the EU carries with it an obligation to comply with many post-authorization organizational and behavioral regulations
relating to the marketing and other activities of authorization holders. These include requirements relating to post-authorization
efficacy studies, post-authorization safety studies, adverse event reporting and other pharmacovigilance requirements, advertising,
packaging and labeling, patient package leaflets, distribution and wholesale dealing. The regulations frequently operate within
a criminal law framework and failure to comply with the requirements may not only affect the authorization, but also can lead to
financial and other sanctions levied on the company in question and responsible officers.
As a result of the currently on-going overhaul
of EU pharmacovigilance legislation the financial and organizational burden on market authorization holders will increase significantly,
such as the obligation to maintain a pharmacovigilance system master file that applies to all holders of marketing authorizations
granted in accordance with Directive 2001/83/EC or Regulation (EC) No 726/2004. Marketing authorization holders must furthermore
collect data on adverse events associated with use of the authorized product outside the scope of the authorization. Pharmacovigilance
for biological products and medicines with a new active substance will be strengthened by subjecting their authorization to additional
monitoring activities. The EU is currently in the process of issuing implementing regulations for the new pharmacovigilance framework.
Any authorization granted by member state
authorities, which within three years of its granting is not followed by the actual placing on the market of the authorized product
in the authorizing member state ceases to be valid. When an authorized product previously placed on the market in the authorizing
member state is no longer actually present on the market for a period of three consecutive years, the authorization for that product
shall cease to be valid. The same two three year periods apply to authorizations granted by the European Commission based on the
In addition to regulations of other countries
where we are seeking or will seek regulatory approval, Israeli government regulations will also govern the development of our product
Clinical Testing in Israel
In order to conduct clinical testing on
humans in Israel, special authorization must first be obtained from the ethics committee and general manager of the institution
in which the clinical studies are scheduled to be conducted, as required under the Guidelines for Clinical Trials in Human Subjects
implemented pursuant to the Israeli Public Health Regulations (Clinical Trials in Human Subjects), as amended from time to time,
and other applicable legislation. These regulations also require authorization from the Israel Ministry of Health, except in certain
circumstances, and in the case of genetic trials, special fertility trials and similar trials, an additional authorization of the
overseeing institutional ethics committee. The institutional ethics committee must, among other things, evaluate the anticipated
benefits that are likely to be derived from the project to determine if it justifies the risks and inconvenience to be inflicted
on the human subjects, and the committee must ensure that adequate protection exists for the rights and safety of the participants
as well as the accuracy of the information gathered in the course of the clinical testing. Since we intend to perform a portion
of the clinical studies on certain of our therapeutic candidates in Israel, we will be required to obtain authorization from the
ethics committee and general manager of each institution in which we intend to conduct our clinical trials, and in most cases,
from the Israel Ministry of Health.
Israel Ministry of Health
Israel’s Ministry of Health, which
regulates medical testing, has adopted protocols that correspond, generally, to those of the FDA and the EMA, making it comparatively
straightforward for studies conducted in Israel to satisfy FDA and the EMA requirements, thereby enabling medical technologies
subjected to clinical trials in Israel to reach U.S. and EU commercial markets in an expedited fashion. Many members of Israel’s
medical community have earned international prestige in their chosen fields of expertise and routinely collaborate, teach and lecture
at leading medical centers throughout the world. Israel also has free trade agreements with the United States and the European
In addition to regulations of other countries
where we are seeking or will seek regulatory approval, Ukrainian government regulations will also govern the development of our
The Ukrainian legislation on registration
and marketing of the medicinal products has been harmonized with the EU legislation since 2005. The general requirements for documentation
and expert evaluation process are fairly close to the European directives, although there are national requirements which may significantly
affect regulatory process.
The national legislation on registration
of the medicinal products is very closely intertwined with the requirements for safety (pharmacovigilance) and quality management.
Therefore, in order to obtain and maintain the Registration Certificate for the finished medicinal product, the applicant has to:
|●||conduct state registration by submitting the application to the Ministry
of Health of Ukraine and by expert evaluation of the documents of the registration dossier in the SEC;|
|●||establish and maintain the pharmacovigilance system in Ukraine;|
|●||confirm or certify the manufacturing compliance with the GMP requirements;
|●||register the layouts (artworks) of the primary and secondary packaging
in the Unified Automated Information System (“UAIS”) of the State Service of Ukraine on Medicines and Drugs Control
a resident and a non-resident of Ukraine (for example, the manufacturer himself) may act as a Marketing Authorization Holder (“MAH”)
for registration. In accordance with the law it is the MAH who has responsibility for the quality, safety and efficacy of the medicinal
product during marketing within the territory of Ukraine. If the MAH and the manufacturer are different entities, it is necessary
to include the documentation clarifying association between them in the registration materials.
non-resident MAH does not have to establish a local representative office or another corporate entity within the territory of Ukraine.
However, the MAH is obliged to establish and maintain the pharmacovigilance system in Ukraine, including the necessity to appoint
the local contact person responsible for pharmacovigilance and to appoint the person in Ukraine, who will be responsible for the
medicinal product quality.
Ministry of Health of Ukraine (the “MOH”) is the central executive body of the healthcare system. The MOH accepts
the applications for the medicinal product registration and approves decisions on registration by issuing Orders.
State Expert Center of the Ministry of Health of Ukraine examines the registration dossiers during registration procedure and
supervises the medicinal products safety (pharmacovigilance).
SMDC implements the state policy on quality control of the medicinal products and medical devices, carries out activities
on recognition (certification) of manufacturing compliance with the GMP requirements.
Documentation and Procedure
documentation for the standard new registration procedure consists of the following parts:
|●||Application for registration, completed according to the national
|●||Registration form (legal and administrative documentation that accompanies
|●||Registration dossier in Common Technical Document (“CTD”)
format, consisting of 5 Modules (Modules 2-5 meet the International Council for Harmonisation of Technical Requirements for Pharmaceuticals
for Human Use (ICH) CTD requirements);|
|●||Translation of registration dossier parts into Ukrainian or Russian;
|●||Specific national documents, namely:|
|o||QCMs are the quality control methods for the medicinal product that include the medicinal product composition, release and
storage specifications, detailed method descriptions, data on the manufacturers, packaging description, shelf-life and storage
|o||Instruction for medical use is the information on use of the medicinal product, which is most often supplied as a leaflet;
|o||Layout and description of the packaging is the description of the information on the primary and secondary packaging of the
registration procedure and the review of application dossier in Ukraine is similar to the EU model. For example, the review of
full dossier takes 210 days. Following the first (initial) registration, the Registration Certificate is issued for a period of
5 years. Not later than 90 days before the end of registration period (5 years), the application for re-registration may be submitted
(the recommended deadline is 10-11 months in advance). After the re-registration, the Registration Certificate of unlimited duration
is issued (unless the MOH decides to conduct an additional re-registration after 5 years for valid reasons related to pharmacovigilance).
re-registration significantly fewer documents are required, compared to initial registration. During re-registration the main focus
is on the management of the medicinal product safety, that is, on the documents of the pharmacovigilance system and the Instruction
for medical use of the medicinal product. Before submitting the application for re-registration, it is necessary to submit separate
applications for all of the changes. These submitted applications (changes and re-registration) are examined in parallel, and independently
of each other.
Ukraine, it is allowed to advertise non-prescription (“OTC”) medicinal products only. Advertising the prescription
medicinal products in non-specialized media is prohibited. There are rigorous restrictions regarding the OTC medicinal products
advertising, most of which are described in Article 21 of the Law of Ukraine “On Advertising”, and there are also other
legislative restrictions. The promotion of prescription medicinal products is allowed in specialized publications intended for
medical institutions and doctors, as well as for distribution at seminars, conferences, symposiums on medical topics.
the regulatory environment for the medicinal products in China has been considered a challenging one, due to:
|●||discrepancies between national and international quality standards;
|●||timeframes for review and approval of new drugs that is longer than
in most major countries; and |
|●||a lack of capacity of the regulatory bodies that has resulted in a
backlog of applications. |
August 2015, the China State Council issued “Opinions on Reforming the Review and Approval System for Drugs and Medical Devices.”
The overarching intention of this initiative was to promote transformation and upgrade of the pharmaceutical industry and bring
marketed products up to international standards in terms of efficacy, safety and quality, so as to better meet the public needs
for drugs. For future NDAs, the CFDA requires applicants to include a clinical trial self-inspection report, which the CFDA will
February 2016, the CFDA initiated a priority review procedure, pursuant to which the following medicinal product categories will
be eligible for the priority review status:
|●||Innovative drugs not approved anywhere worldwide;|
|●||Innovative drugs where there is a plan to transfer the manufacturing
site to China;|
|●||Global clinical trial application (“CTA”) to China in
parallel with the US or EU;|
|●||Innovative drugs for HIV/AIDS, viral hepatitis, rare disease(s), malignant
tumors and pediatric indications; and|
|●||Newly launched generic drugs. |
the CFDA approves the priority review process request, applicants are given priority reviewer resources allocated by the Center
for Drug Evaluation (“CDE”) and additional channels to communicate with and obtain quick feedback from the CDE/CFDA.
Target approval time from submission is within six months.
started to implement a pilot program MAH System in ten provinces in 2015. The MAH system will be implemented throughout China
and the Drug Administration Law of China will be amended accordingly. Under such program, a research and development organization
or its personnel can be an MAH. The MAH will be fully responsible for any liability with respect to the drug during the lifecycle.
The parties authorized by the MAH to conduct relevant work, including research and production, will bear liability in accordance
with the law and the applicable agreements. In addition, the MAH will also be required to establish a system to directly report
adverse drug reactions or adverse drug events.
has also created a new classification “new to the world”, to replace the previous “new to China” category.
This is based on the global marketing authorization approval status and the location of the manufacturing sites inside or outside
of China. This removes the previous definitions that were based on the specific status in China and aligns classification more
closely to other regulatory agencies.
October 10, 2017, the CFDA issued the Decision to Adjust Relevant Items concerning Imported Drug Registration (the "Imported
Drug Decision"). The Imported Drug Decision implemented changes to facilitate the review and approval process for imported
drugs, particularly for innovative imported drugs. Pursuant to the Imported Drug Decision, the CFDA will accept foreign clinical
trial data as part of international multi-center clinical trials. In addition, the Imported Drug Decision provides that an overseas
applicant intending to conduct an international multi-center clinical trial in China can simultaneously conduct a Phase I clinical
trial inside and outside China, which essentially means foreign Phase I clinical trial data can be used for the approval application
of imported drugs.
The Submission Policy
Previously, the CFDA required that a foreign-developed
drug must be approved in another country, and then proceed to China for NDA/MAA submission. Even if there is multinational clinical
trial (“MNCT”) data in China, the applicant had to wait for the Certificates of Pharmaceutical Product (“CPP”)
from the US, EU or other countries, and only then could there be a second submission (submission to the CFDA to request clinical
Under the new policy, there is no need for
the CPP. After completing the MNCT with the necessary relevant clinical study report (CSR), a sponsor can make an NDA/MAA submission
to the CFDA without CPP. This means, theoretically, that the China NDA/MAA submission and approval can be in parallel with (or
even precede) the foreign MAA approval. These changes more closely align China to global standards, processes and timelines and
should have a substantial impact on the China local pharmaceutical market and on the global pharmaceutical industry.
This new policy is expected to have a strong
positive impact on foreign-developed new drug innovators who can have a full clinical development program inside China, with significantly
shortened regulatory review processes. The CFDA marketing authorization approval can be in parallel with the US, EU or any other
During 2017, the CFDA announced the following
policies which may also positively impact the product registration process in China:
|●||Policy on reform of clinical trial management. The CFDA will no longer
accredit clinical sites with GCP. This opens clinical sites to all qualified hospitals, meaning a likely increase in the number
of sites able to manage clinical trials in order to meet the need of increase of drug and medical device trials in China. The CFDA
retains responsibility for site inspections.|
|●||Policy on acceleration of drug and medical device registration review
process. For medicinal products indicated for serious life-threatening conditions or for significant unmet medical needs, where
early or mid-stage clinical data can predict clinical benefits, the CFDA will be able to grant a conditional approval to allow
early marketing in China, with a defined risk management plan and commitment to complete required clinical trial(s) based on the
CFDA’s review and conclusion. China’s Ministry of Health will issue a rare disease list for China and set up a rare
disease patient registration process. The orphan drug and medical device manufacturer/applicant can apply for a clinical trial
waiver or an agreed decrease in trial subject numbers. For orphan drugs or medical devices that are already approved outside of
China, the CFDA can issue a conditional approval to allow marketing in China, while the sponsor completes commitment for clinical
trial based on the CFDA’s review and conclusion.|
In general, positive changes for China’s
regulatory environment are expected to better align China with global regulatory norms by achieving the following:
|●||Shortening the new IND and NDA review timeline. This may reverse
the previous reluctance to include China in global studies or programs because of the long IND timelines.|
|●||Increasing transparency and globalization. The CFDA is encouraging
foreign sponsors to undertake global studies in China and recommending that local clinical sites join global studies to help ensure
clinical trial data meet the requirements needed for China and global registration. |
|●||Minimizing the drug lag. The change in the foreign drug registration
process by eliminating the CPP requirement may allow the drug approval process in China to be in parallel with the US and/or the
In addition to regulations in the United
States, the EU, Israel, Ukraine and China, we may be subject to a variety of other regulations governing clinical trials and commercial
sales and distribution of drugs in other countries. Whether or not our products receive approval from the FDA or EMA approval of
such products must be obtained by the comparable regulatory authorities of countries other than the United States or European Union
before we can commence clinical trials or marketing of the product in those countries. The approval process varies from country
to country, and the time may be longer or shorter than that required for FDA or EMA approval. The requirements governing the conduct
of clinical trials and product licensing vary greatly from country to country.
The requirements that we and our collaborators
must satisfy to obtain regulatory approval by government agencies in other countries prior to commercialization of our products
in such countries can be rigorous, costly and uncertain. In the European countries, Canada and Australia, regulatory requirements
and approval processes are similar in principle to those in the United States. Additionally, depending on the type of drug
for which approval is sought, there are currently two potential tracks for marketing approval in the European countries: mutual
recognition and the centralized procedure. These review mechanisms may ultimately lead to approval in all European Union
countries, but each method grants all participating countries some decision-making authority in product approval. Foreign
governments also have stringent post-approval requirements including those relating to manufacture, labeling, reporting, record
keeping and marketing. Failure to substantially comply with these on-going requirements could lead to government action against
the product, us and/or our representatives.
From time to time, legislation is drafted,
introduced and passed in governmental bodies that could significantly change the statutory provisions governing the approval, manufacturing
and marketing of products regulated by the FDA or EMA and other applicable regulatory bodies to which we are subject. In addition,
regulations and guidance are often revised or reinterpreted by the national agency in ways that may significantly affect our business
and our therapeutic candidates. It is impossible to predict whether such legislative changes will be enacted, whether FDA or EMA
regulations, guidance or interpretations will change, or what the impact of such changes, if any, may be. We may need to adapt
our business and therapeutic candidates and products to changes that occur in the future.
Our business and operations are generally
not affected by seasonal fluctuations or factors.
Implications of Being an Emerging
We qualify as an “emerging growth
company” as defined in the Jumpstart Our Business Startups Act of 2012, or the JOBS Act. As an emerging growth company, we
may take advantage of specified reduced disclosure and other requirements that are otherwise applicable generally to public companies.
These provisions include:
||a requirement to provide only two years of audited financial statements in addition to any required unaudited interim financial statements with correspondingly reduced “Management’s Discussion and Analysis of Financial Condition and Results of Operations” disclosure;|
||reduced disclosure about executive compensation arrangements;|
||no non-binding advisory votes on executive compensation or golden parachute arrangements; and |
||an exemption from the auditor attestation requirement in the assessment of internal control over financial reporting.|
We may take advantage of these provisions
for up to five years or such earlier time that we are no longer an emerging growth company. We would cease to be an emerging growth
company on the date that is the earliest of (i) the last day of the fiscal year in which we had total annual gross revenues of
$1 billion or more; (ii) the last day of our fiscal year following the fifth anniversary of the date of the completion of our initial
public offering; (iii) the date on which we had issued more than $1 billion in nonconvertible debt during the previous three years;
or (iv) the date on which we are deemed to be a large accelerated filer under the rules of the SEC.
To the extent that we continue to qualify
as a “smaller reporting company,” as such term is defined in Rule 12b-2 under the Exchange Act, after we cease to qualify
as an emerging growth company, certain of the exemptions available to us as an emerging growth company may continue to be available
to us as a smaller reporting company, including: (1) not being required to comply with the auditor attestation requirements of
Section 404(b) of the Sarbanes Oxley Act; (2) scaled executive compensation disclosures; and (3) the requirement to provide only
two years of audited financial statements, instead of three years.
We currently have one full time employee,
Or Eisenberg, our Acting Chief Executive Officer and Chief Financial Officer, and one part time employee. In addition, our Chief
Operating Officer dedicates 80% of his time to us and our Chairman of the Board commits 20% of his time to us, both engaged by
us via such persons’ wholly owned services companies. In addition, we engage certain outside consultants that are, in general,
compensated on an hourly basis.
ITEM 1A. RISK FACTORS.
An investment in our securities
involves a high degree of risk. You should consider carefully the following information about these risks, together with the
other information contained in this Annual Report, including the matters addressed in the section entitled “CAUTIONARY
STATEMENT REGARDING FORWARD-LOOKING STATEMENTS,” beginning on page ii of this Annual Report, before making an
investment decision. Our business, prospects, financial condition, and results of operations may be materially and adversely
affected as a result of any of the following risks. The value of our securities could decline as a result of any of these
risks. You could lose all or part of your investment in our securities. Some of the statements in “RISK FACTORS”
are forward-looking statements. The following risk factors are not the only risk factors facing our company. Additional risks
and uncertainties not presently known to us or that we currently deem immaterial may also affect our business, prospects,
financial condition, and results of operations and it is not possible to predict all risk factors, nor can we assess the
impact of all factors on us or the extent to which any factor or combination of factors may cause actual results to differ
materially from those contained in or implied by any forward-looking statements.
Risks Related to our Business
We have incurred operating losses
since our inception and anticipate that we will continue to incur substantial operating losses for the foreseeable future.
We are a clinical-stage biopharmaceutical
company currently focused on the treatment of ophthalmic disorders, including DES. We have in-licensed certain rights to LO2A,
a drug developed for the treatment of DES, and other ophthalmological illnesses, including CCH and Sjögren’s. Since
April 2015, we have been financing our operations through numerous financing activities, including the issuance of ordinary shares
and from loans from Ridge and Rimon Gold Rimon Gold and from third parties. We have historically incurred net losses, including
net losses of approximately $2.97 million and $1.1 million for the years ended December 31, 2017 and 2016, respectively. At December
31, 2017, we had an accumulated deficit of approximately $26.4 million. We do not know whether or when we will become profitable.
To date, we have not commercialized any products or generated any revenues from product sales and accordingly we do not have a
revenue stream to support our cost structure. Our losses have resulted principally from costs incurred in development and discovery
activities as well as from certain financial expenses related mainly to convertible loans. We expect to continue to incur losses
for the foreseeable future, and these losses will likely increase as we:
||initiate and manage pre-clinical development and clinical trials for LO2A;|
||seek regulatory approvals for LO2A;|
||implement internal systems and infrastructures;|
||seek to license additional technologies to develop;|
||pay royalties and other payments related to the LO2A License Agreement;|
||hire management and other personnel; and|
||move towards commercialization.|
No certainty exists that we will be able
to complete the development of LO2A for CCH, Sjögren’s or any other ophthalmic disorder, due to financial, technological
or other difficulties. If LO2A fails in clinical trials or does not gain regulatory clearance or approval, or if LO2A does not
achieve market acceptance, we may never become profitable. Even if we do achieve profitability, we may not be able to sustain or
increase profitability on a quarterly or annual basis. Our inability to achieve and then maintain profitability would negatively
affect our business, financial condition, results of operations and cash flows. Moreover, our prospects must be considered in light
of the risks and uncertainties encountered by an early-stage company and in highly regulated and competitive markets, such as the
biopharmaceutical market, where regulatory approval and market acceptance of our products are uncertain. There can be no assurance
that our efforts will ultimately be successful or result in revenues or profits.
We have substantial debt which may
adversely affect us by limiting future sources of financing, interfering with our ability to pay interest and principal on the
Convertible Loans and subjecting us to additional risks.
We have a significant amount of indebtedness.
As of December 31, 2017, we had a total of $1,415,323 of loans (principal and interest) outstanding under Convertible Loans, of
which (1) Ridge extended a principal amount of $274,048, (2) Rimon Gold extended a principal amount of $805,115, and (3) Fisher
extended a principal amount of $274,048. If we incur additional indebtedness to our current indebtedness levels, including other
short or long-term credit facilities, the related risks that we now face could increase. For more information relating to the
Convertible Loans and the agreements relating thereto, please see Item 7 - “MANAGEMENT’S DISCUSSION AND ANALYSIS OF
FINANCIAL CONDITION AND RESULTS OF OPERATIONS,” beginning on page 62 of this Annual Report.
Our substantial debt could have important
||making it more difficult for us to satisfy our obligations with respect to the Convertible Loans and other obligations;|
||limiting our ability to obtain additional financing on satisfactory terms and to otherwise fund working capital, capital expenditures, and other general corporate requirements;|
||our ability to adjust to changing market conditions;|
||increasing our vulnerability to general adverse economic and industry conditions;|
||placing us at a competitive disadvantage compared to our competitors that have no debt or are less leveraged;|
||limiting our flexibility in planning for, or reacting to, changes in our business and the industry in which we operate; and|
||restricting us from making strategic acquisitions or exploiting business opportunities.|
Our assets are subject to security
interests in favor of Rimon Gold. Our failure to repay the Convertible Loans, if required, could result in legal action against
us, which could require the sale of all of our assets.
In order to secure our obligations and performance
pursuant to the Convertible Loans from Rimon Gold, we recorded a first priority fixed charge in favor of Rimon Gold on all of our
rights, including our distribution rights, under the LO2A License Agreement, and a first priority floating charge on all of our
rights, title and interest in all of our assets, as exist from time to time. If we are unable to repay the Convertible Loans from
Rimon Gold when due, Rimon Gold could foreclose on our assets in order to recover the amounts due. Any such action would require
us to curtail or cease operations.
The Convertible Loans contain restrictive
covenants that may limit our corporate activities, which could have an adverse effect on our financial condition and results
We delivered to Rimon Gold an Irrevocable
Guaranty and Undertaking (the “Wize Guaranty”) pursuant to which we irrevocably guarantee Wize Israel’s obligations
to Rimon Gold under the Convertible Loans. The Wize Guaranty contains a number of restrictive covenants that limit our operating
flexibility. Furthermore, the Convertible Loans (including the Security Agreements associated therewith) contain a number of undertakings
and restrictive covenants that, until the full repayment of such loans (including by way of conversion into our shares), limit
our operating and financial flexibility. The covenants in the Convertible Loans (including the Security Agreements associated therewith)
and the Wize Guaranty include, among other things, limitations on the creations of liens; on the incurrence of indebtedness; on
dispositions of assets, mergers, acquisitions and change of control transactions; on changes in the general nature of our business;
and on the distribution of dividends. Such obligations may hinder our future operations or the manner in which we operate our business,
which could have a material adverse effect on our business, financial condition or results of operations. These restrictions could
also limit our ability to plan for or react to market conditions or meet extraordinary capital needs or otherwise restrict corporate
activities. These provisions, when taken as a whole, may also have the effect of making an acquisition of us more difficult
and, consequently, also cause our shares to trade at prices below the price for which third parties might be willing to pay to
gain control of us.
As a result of the restrictions in the Convertible
Loans (including the Security Agreements associated therewith) and the Wize Guaranty, or similar restrictions in our future financing
arrangements, we may need to seek permission from our lenders in order to engage in certain corporate actions. Our lenders’
interests may be different from ours and we may not be able to obtain their permission when needed or at all. This may prevent
us from taking actions that we believe are in our best interest, which may adversely impact our revenues, results of operations
and financial condition.
We will need to raise additional capital
to meet our business requirements in the future, and such capital raising may be costly or difficult to obtain and will dilute
current stockholders’ ownership interests.
The sources of financing at our disposal
are estimated by our management to be currently insufficient (i) to conduct our ongoing business for the next 12 months, (ii) to
conduct any future clinical trials, and (iii) for LO2A’s commercial production and marketing. No certainty exists that we
will be able to secure the additional sources of finance we need to perform the advanced and necessary stages of receiving regulatory
approvals for marketing and distributing our products, including the costs derived from performing clinical trials and the requirements
of the regulatory authorities. The lack of satisfactory means of financing may bring our business activity to a halt. As of December
31, 2017, we had cash and cash equivalents of approximately $215,000. We have expended and believe that we will continue to expend
substantial resources for the foreseeable future developing LO2A. These expenditures will include costs associated with research
and development, manufacturing, conducting clinical trials, as well as commercializing any products approved for sale. Because
the outcome of our planned and anticipated clinical trials is highly uncertain, we cannot reasonably estimate the actual amounts
necessary to successfully complete the development and commercialization of LO2A. In addition, other unanticipated costs may arise.
As a result of these and other factors currently unknown to us, we will require additional funds, through public or private equity
or debt financings or other sources, such as strategic partnerships and alliances and licensing arrangements. In addition, we may
seek additional capital due to favorable market conditions or strategic considerations even if we believe we have sufficient funds
for our current or future operating plans.
Our future capital requirements will depend
on many factors, including the progress and results of our clinical trials, the duration and cost of discovery and preclinical
development, and laboratory testing and clinical trials of LO2A, the timing and outcome of regulatory review of LO2A, the number
and development requirements of other product candidates that we pursue, if any, and the costs of activities, such as product marketing,
sales, and distribution. Because of the numerous risks and uncertainties associated with the development and commercialization
of LO2A, we are unable to estimate the amounts of increased capital outlays and operating expenditures associated with our anticipated
Our future capital requirements depend on
many factors, including:
||the need to service debt obligations under the Convertible Loans;|
||any payments to be made to Resdevco under the LO2A License Agreement;|
||the failure to obtain regulatory approval or achieve commercial success of LO2A;|
||the results of our preclinical studies and clinical trials for any future earlier stage product candidate, and any decisions to initiate clinical trials if supported by the preclinical results;|
||the costs, timing and outcome of regulatory review of LO2A that progress to clinical trials;|
||the costs of preparing, filing and prosecuting patent applications, maintaining and enforcing our issued patents and defending intellectual property-related claims;|
||the cost of commercialization activities if any LO2A is approved for sale for a particular indication, including marketing, sales and distribution costs;|
||the cost of manufacturing LO2A;|
||the timing, receipt and amount of sales of, or royalties on, our future products, if any;|
||the expenses needed to attract and retain skilled personnel;|
||any product liability or other lawsuits related to our products;|
||the extent to which we acquire or invest in businesses, products or technologies and other strategic relationships; and|
||the costs of financing unanticipated working capital requirements and responding to competitive pressures. |
Additional funds may not be available when
we need them, on terms that are acceptable to us, or at all. If adequate funds are not available to us on a timely basis, we may
be required to delay, limit, reduce or terminate preclinical studies, clinical trials or other research and development activities
for LO2A or delay, limit, reduce or terminate our establishment of sales and marketing capabilities or other activities that may
be necessary to commercialize LO2A.
We may incur substantial costs in pursuing
future capital financing, including investment banking fees, legal fees, accounting fees, securities law compliance fees, printing
and distribution expenses and other costs. We may also be required to recognize non-cash expenses in connection with certain securities
we issue, such as convertible notes and warrants, which may adversely impact our financial condition.
According to management estimates,
liquidity resources as of December 31, 2017 will not be sufficient to maintain our operations for the next twelve months which
raises substantial doubt regarding our ability to continue as a going concern. If we do not continue as a going concern, investors
could lose their entire investment.
According to management estimates, liquidity
resources as of December 31, 2017, will not be sufficient to maintain our operations for the next 12 months. Our inability to
raise funds to conduct our research and development activities will have a severe negative impact on our ability to remain a viable
company. These conditions raise substantial doubt about our ability to continue as a going concern. As such, the report of our
independent registered public accounting firm on our audited financial statements as of and for the year ended December 31, 2017
contains an emphasis of matter paragraph regarding substantial doubt about our ability to continue as a going concern. This emphasis
of matter paragraph could materially limit our ability to raise additional funds through the issuance of debt or equity securities
or otherwise. Future reports on our annual financial statements may include an emphasis of matter paragraph with respect to our
ability to continue as a going concern.
If we fail to obtain necessary funds
for our operations, we will be unable to maintain and improve our licensed technology, and we will be unable to develop and commercialize
Our present and future capital requirements
depend on many factors, including:
||the level of research and development investment required to develop LO2A;|
||the costs of obtaining or manufacturing LO2A for research and development and testing;|
||the results of preclinical and clinical testing, which can be unpredictable in drug development;|
||changes in drug development plans needed to address any difficulties that may arise in manufacturing, preclinical activities or clinical studies;|
||our ability and willingness to enter into new agreements with strategic partners and the terms of these agreements;|
||our success rate in preclinical and clinical efforts associated with milestones and royalties;|
||the costs of investigating patents that might block us from developing potential product candidates;|
||the costs of recruiting and retaining qualified personnel;|
||the time and costs involved in obtaining regulatory approvals;|
||the costs of filing, prosecuting, defending and enforcing patent claims and other intellectual property rights; and|
||our need or decision to acquire or license complementary technologies or new platform or product candidate targets. |
If we are unable to obtain the funds necessary
for our operations, we will be unable to maintain and improve our licensed technology, and we will be unable to develop and commercialize
our products and technologies, which would materially and adversely affect our business, liquidity and results of operations.
Potential administrative enforcement
proceedings may have an adverse effect on our business and financial condition.
To our knowledge, the Israel Securities
Authority (the “ISA”) is conducting an administrative inquiry regarding Wize Israel’s public reports with the
ISA in Israel regarding its applicable regulatory path necessary for the marketing of LO2A for the treatment of DES in the United
States. As part of the inquiry, the ISA requested Wize Israel to provide certain documentation and has also questioned its
officers with respect to such reports. Wize Israel and its officers cooperated with the ISA and, at the ISA’s request, Wize
Israel also publicly filed a supplemental report to provide additional information in connection with the said regulatory path
and marketing plans, which we believe contained all the required information. As of the date of this Annual Report, it is uncertain
whether such inquiry will lead to any administrative enforcement proceedings by the ISA, if at all. In the event the ISA commences
enforcement proceedings against Wize Israel or its office holders, this could result, among other things, in financial sanctions
against Wize Israel or its office holders, which can adversely effect our business and financial condition.
Risks Related to our Business and Regulatory
We have not yet commercialized LO2A,
and may never become profitable.
Although LO2A is approved for sale for certain
indications in a limited number of jurisdictions, we have not yet commenced commercialization of LO2A, and may never be able to
do so other than with respect to the entry into of distribution agreements in Israel and Ukraine, which are not expected to result
in material revenues. Our activity is influenced by the policies of regulatory authorities. Changes and developments in regulatory
requirements or our failure to meet such requirements may lead to restrictions or delays in developing LO2A and cause material
expenses for us. We do not know when or if we will complete any of our product development efforts of LO2A, obtain regulatory approval
for any future product candidates incorporating our technologies or successfully commercialize any approved products. Even if we
are successful in developing LO2A that is approved for marketing, we will not be successful unless these products gain market acceptance
for appropriate indications at favorable reimbursement rates. The degree of market acceptance of these products will depend on
a number of factors, including:
||the timing of regulatory approvals in the countries, and for the uses, we seek;|
||the competitive environment;|
||the establishment and demonstration in the medical community of the safety and clinical efficacy of LO2A and its potential advantages over existing therapeutic products;|
||our ability to enter into strategic agreements with pharmaceutical and biotechnology companies with strong marketing and sales capabilities;|
||the adequacy and success of distribution, sales and marketing efforts; and|
||the pricing and reimbursement policies of government and third-party payors, such as insurance companies, health maintenance organizations and other plan administrators.|
Physicians, patients, thirty-party payors
or the medical community in general may be unwilling to accept, utilize or recommend, and in the case of third-party payors, cover
any of our products or products incorporating our technologies. As a result, we are unable to predict the extent of future losses
or the time required to achieve profitability, if at all. Even if we successfully develop one or more products that incorporate
our technologies, we may not become profitable.
Our current pipeline is based on a
single compound, LO2A. Failure to develop LO2A will have a material adverse effect on us.
In August 2016, we commenced a Phase II
randomized, double-blind, placebo-controlled, clinical trial, in parallel groups which is intended for the repeated confirmation
of the effectiveness and safety of LO2A for patients suffering from moderate to severe CCH. The Multi-Center Trial is in five
different medical centers in Israel with only us having access to the trial data. As of March 26, 2018, the Multi-Center Trial
had already enrolled all the planned 62 patients, with the treatment time for each patient being three months.
On October 26, 2017, Wize Israel announced
the termination of its Single-Center Trial in Israel that commenced in January 2017. The Single Center Trial was a Phase II, randomized,
double-blind, placebo-controlled, pilot study carried out in parallel groups that was intended to evaluate the safety and efficacy
of LO2A for patients suffering from moderate to severe CCH with Wize Israel having sole access to the trial data. On October 24,
2017, Wize Israel received notice from the CRO that manages and supervises Wize Israel’s clinical trials, that an inadequate
amount of quality information may be derived from the results collected thus far, given that there is no correlation in the reaction
of both eyes to LO2A, in contrast to professional literature and other trials. In addition, the recruitment rate of patients was
less than required and there was a higher than expected dropout rate. In light of the above, the CRO concluded that the results
of the trial would be of no use even if the trial continued until the end of its term. Based on the CRO’s conclusion, Wize
Israel determined to terminate the trial and to save the future costs that would be incurred in connection with such trial.
LO2A is at various stages of clinical development
and may never be commercialized for the indications in the territories that we presently have rights under the LO2A License Agreement.
The progress and results of any future clinical trials are uncertain, and the failure of LO2A to receive regulatory approvals will
have a material adverse effect on our business, operating results and financial condition to the extent we are unable to commercialize
LO2A. In addition, we face the risks of failure inherent in developing therapeutic products.
Furthermore, LO2A must satisfy rigorous
standards of safety and efficacy before it can be approved by the U.S. Food and Drug Administration (the “FDA”), and
any applicable foreign regulatory authorities for commercial use. The FDA and foreign regulatory authorities have full discretion
over this approval process. We will need to conduct significant additional research, involving testing in animals and in humans,
before we can file applications for product approval. Typically, in the pharmaceutical industry, there is a high rate of attrition
for product candidates in pre-clinical testing and clinical trials. Also, satisfying regulatory requirements typically takes many
years, is dependent upon the type, complexity and novelty of the product and requires the expenditure of substantial resources.
In addition, delays or rejections may be encountered based upon additional government regulation, including any changes in FDA
policy, during the process of product development, clinical trials and regulatory reviews.
In order to receive FDA approval or approval
from foreign regulatory authorities to market a product candidate, we must demonstrate through pre-clinical testing and through
human clinical trials that the product candidate is safe and effective for its intended uses (e.g., treatment of a specific
condition in a specific way subject to contradictions and other limitations). Even if we comply with all FDA requests, the FDA
may ultimately reject one or more of our NDAs or grant approval for a narrowly intended use that is not commercially feasible.
We might not obtain regulatory approval for LO2A in a timely manner, if at all. Failure to obtain FDA approval for
LO2A in a timely manner or at all will severely undermine our business by reducing the number of salable products and, therefore,
corresponding product revenues.
Results of earlier clinical trials
may not be predictive of the results of later-stage clinical trials.
The results of preclinical studies and early
clinical trials of product candidates may not be predictive of the results of later-stage clinical trials. Product candidates in
later stages of clinical trials may fail to show the desired safety and efficacy results despite having progressed through preclinical
studies and initial clinical trials. Many companies in the pharmaceutical industry have suffered significant setbacks in advanced
clinical trials due to adverse safety profiles or lack of efficacy, notwithstanding promising results in earlier studies. Any delay
in, or termination or suspension of, our clinical trials will delay the requisite filings with the FDA or any applicable foreign
regulatory authority and, ultimately, our ability to commercialize LO2A and generate product revenues. If the clinical trials
do not support our product claims, the completion of development of such product candidates may be significantly delayed or abandoned,
which will significantly impair our ability to generate product revenues and will materially adversely affect our results of operations.
This drug candidate development risk is
heightened by any changes in the planned clinical trials compared to the completed clinical trials. As product candidates are developed
from preclinical through early to late stage clinical trials towards approval and commercialization, it is customary that various
aspects of the development program, such as manufacturing and methods of administration, are altered along the way in an effort
to optimize processes and results. While these types of changes are common and are intended to optimize the product candidates
for late stage clinical trials, approval and commercialization, such changes do carry the risk that they will not achieve these
Changes in our clinical trials or future
clinical trials could cause LO2A or any future product candidate to perform differently, including causing toxicities, which could
delay completion of our clinical trials, delay approval of our product candidates, and/or jeopardize our ability to commence product
sales and generate revenues.
We might be unable to develop LO2A
that will achieve commercial success in a timely and cost-effective manner, or ever.
Even if regulatory authorities approve LO2A
for the indications in the territories that we presently have rights under the LO2A License Agreement, they may not be commercially
successful. LO2A may not be commercially successful because government agencies and other third-party payors may not cover the
product or the coverage may be too limited to be commercially successful; physicians and others may not use or recommend our products,
even following regulatory approval. A product approval, assuming one issues, may limit the uses for which the product may be distributed
thereby adversely affecting the commercial viability of the product. Third parties may develop superior products or have proprietary
rights that preclude us from marketing our products. Patient acceptance of and demand for LO2A for which we obtain regulatory approval
or license will depend largely on many factors, including but not limited to the extent, if any, of reimbursement of costs by government
agencies and other third-party payors, pricing, the effectiveness of our marketing and distribution efforts, the safety and effectiveness
of alternative products, and the prevalence and severity of side effects associated with our products. If physicians, government
agencies and other third-party payors do not accept our products, we will not be able to generate significant revenue.
Clinical trials are very expensive,
time-consuming and difficult to design and implement, and, as a result, we may suffer delays or suspensions in future trials which
would have a material adverse effect on our ability to generate revenues.
Human clinical trials are very expensive
and difficult to design and implement, in part because they are subject to rigorous regulatory requirements. Regulatory authorities,
such as the FDA, may preclude clinical trials from proceeding. Additionally, the clinical trial process is time-consuming, failure
can occur at any stage of the trials, and we may encounter problems that cause us to abandon or repeat clinical trials.
For example, in October 2017, we terminated
our Single Center Trial. The Single Center Trial was a Phase II, randomized, double-blind, placebo-controlled, pilot study carried
out in parallel groups that was intended to evaluate the safety and efficacy of LO2A for patients suffering from moderate to severe
CCH, with Wize Israel having sole access to the trial data. On October 24, 2017, Wize Israel received notice from the CRO that
manages and supervises Wize Israel’s clinical trials, that an inadequate amount of quality information may be derived from
the results collected thus far, given that there is no correlation in the reaction of both eyes to LO2A, in contrast to professional
literature and other trials. In addition, the recruitment rate of patients was less than required and there was a higher than expected
dropout rate. In light of the above, the CRO concluded that the results of the trial would be of no use even if the trial continued
until the end of its term. Based on the CRO’s conclusion, Wize Israel determined to terminate the trial and to save the future
costs that would be incurred in connection with such trial. For the avoidance of doubt, this does not impact the Multi-Center Trial.
The commencement and completion of clinical
trials may be delayed by several factors, including:
||unforeseen safety issues;|
||determination of dosing issues;|
||lack of effectiveness or efficacy during clinical trials;|
||failure of third party suppliers to perform final manufacturing steps for the drug substance;|
||slower than expected rates of patient recruitment and enrollment;|
||lack of healthy volunteers and patients to conduct trials;|
||inability to monitor patients adequately during or after treatment;|
||failure of third party contract research organizations to properly implement or monitor the clinical trial protocols;|
||failure of institutional review boards to approve our clinical trial protocols;|
||inability or unwillingness of medical investigators and institutional review boards to follow our clinical trial protocols; and|
||lack of sufficient funding to finance the clinical trials. |
We have experienced the risks involved with
conducting clinical trials, including but not limited to, increased expense and delay and failure to meet end points of the trial.
In addition, we or regulatory authorities
may suspend our clinical trials at any time if it appears that we are exposing participants to unacceptable health risks or if
the regulatory authorities find deficiencies in our regulatory submissions or the conduct of these trials. Any suspension of clinical
trials will delay possible regulatory approval, if any, and adversely impact our ability to develop products and generate revenue.
If we acquire or license additional
technology or product candidates, we may incur a number of costs, may have integration difficulties and may experience other risks
that could harm our business and results of operations.
We may acquire and license additional product
candidates and technologies. Any product candidate or technology we license from others or acquire will likely require additional
development efforts prior to commercial sale, including extensive pre-clinical or clinical testing, or both, and approval by the
FDA and applicable foreign regulatory authorities, if any. All product candidates are prone to risks of failure inherent in pharmaceutical
product development, including the possibility that the product candidate or product developed based on licensed technology will
not be shown to be sufficiently safe and effective for approval by regulatory authorities. In addition, we cannot assure you that
any product candidate that we develop based on acquired or licensed technology that is granted regulatory approval will be manufactured
or produced economically, successfully commercialized or widely accepted in the marketplace. Moreover, integrating any newly acquired
product candidates could be expensive and time-consuming. If we cannot effectively manage these aspects of our business strategy,
our business may not succeed.
If any third party upon whom we rely
to manufacture LO2A is unable to timely manufacture LO2A in compliance with current Good Manufacturing Practices (“cGMP”)
and other regulations our business will be harmed.
We do not currently have the ability to
manufacture the compounds that we need to conduct our clinical trials and, therefore, rely upon, and intend to continue to rely
upon, a certain contract manufacturer to produce and supply LO2A (including the active pharmaceutical ingredients, or APIs) for
use in clinical trials and for future sales. If such manufacturer is unable to manufacture the compounds in a timely fashion or
in compliance with current cGMP and other applicable regulations or if there is a strain on the relationship with such manufacturer,
our clinical development programs may be delayed which could have a detrimental effect on our business.
The manufacture of LO2A is a chemical
synthesis process and if our manufacturer encounters problems manufacturing LO2A, our business could suffer.
Regulators throughout the world, including
the FDA, require manufacturers to register manufacturing facilities. Such regulators also inspect these facilities to confirm compliance
with requirements that such regulators establish. We have engaged a contract manufacturer to produce and supply LO2A and such third
party manufacturer may face manufacturing or quality control problems causing product production and shipment delays or a situation
where such manufacturer may not be able to maintain compliance with the applicable regulators’ requirements necessary to
continue manufacturing LO2A. In addition, drug manufacturers may be subject to ongoing periodic unannounced inspections by regulators
to ensure strict compliance with requirements and other regulations and applicable standards. Any failure to comply with such requirements
could adversely affect our clinical research activities and our ability to market and develop LO2A.
We do not currently have sales, marketing
or distribution capabilities or experience, and are unable to effectively sell, market or distribute LO2A now and do not expect
to be able to do so in the future. The failure to enter into agreements with third parties that are capable of performing these
functions would have a material adverse effect on our business and results of operations.
We intend to enter into agreements with
pharmaceutical companies and distributors with relevant marketing capabilities in the field of pharmaceuticals in order to use
them to sell LO2A in countries around the world where we hold rights to sell LO2A. To date, we have entered into two distribution
agreements and one additional framework agreement to market LO2A for DES only. We do not currently have and do not expect to develop
our own sales, marketing and distribution capabilities. If we are unable to enter into agreements with third parties to perform
these functions, we will not be able to successfully market LO2A. In order to successfully market LO2A, we must make arrangements
with third parties to perform these services.
As we do not intend to develop a marketing
and sales force with technical expertise and supporting distribution capabilities, we will be unable to market LO2A directly. To
promote any of our potential products through third parties, we will have to locate acceptable third parties for these functions
and enter into agreements with them on acceptable terms, and may not be able to do so. Any third-party arrangements we are able
to enter into may result in lower revenues than we could achieve by directly marketing and selling our potential products. In addition,
to the extent that we depend on third parties for marketing and distribution, any revenues we receive will depend upon the efforts
of such third parties, as well as the terms of our agreements with such third parties, which cannot be predicted in most cases
at this time. As a result, we might not be able to market and sell LO2A in the United States or overseas, which would have
a material adverse effect on our business.
We face significant competition and
continuous technological change, and developments by competitors may render our products or technologies obsolete or non-competitive.
If we cannot successfully compete with new or existing products, our marketing and sales will suffer and may not ever be profitable.
We are active in a competitive market. The
fierce competition in the field and the introduction of new competitors to the field may negatively impact our monetary results.
We will compete against fully integrated pharmaceutical and biotechnology companies and smaller companies that are collaborating
with larger pharmaceutical companies, academic institutions, government agencies and other public and private research organizations.
In addition, many of these competitors, either alone or together with their collaborative partners, operate larger research and
development programs than ours, and have substantially greater financial resources, as well as significantly greater experience
||undertaking pre-clinical testing and human clinical trials;|
||obtaining FDA, addressing various regulatory matters and other regulatory approvals of drugs;|
||formulating and manufacturing drugs; and|
||launching, marketing and selling drugs. |
If our competitors develop and commercialize
products faster, or develop and commercialize products that are superior to LO2A, our commercial opportunities will be reduced
or eliminated. The extent to which LO2A achieves market acceptance will depend on competitive factors, many of which are beyond
our control. Competition in the biotechnology and biopharmaceutical industry is intense and has been accentuated by the rapid pace
of technology development. Our competitors include large integrated pharmaceutical companies, biotechnology companies that currently
have drug and target discovery efforts, universities, and public and private research institutions. Almost all of these entities
have substantially greater research and development capabilities and financial, scientific, manufacturing, marketing and sales
resources than us. These organizations also compete with us to:
||attract parties for acquisitions, joint ventures or other collaborations;|
||license proprietary technology that is competitive with the technology we are developing;|
||attract and hire scientific talent and other qualified personnel.|
Our competitors may succeed in developing
and commercializing products earlier and obtaining regulatory approvals from the FDA and other foreign regulatory authorities more
rapidly. Our competitors may also develop products or technologies that are superior to those we are developing, and render LO2A
or any future product candidate or technology obsolete or non-competitive. If we cannot successfully compete with new or existing
products, our marketing and sales will suffer and may never be profitable.
We may suffer losses from product
liability claims if LO2A causes harm to patients.
LO2A could cause adverse events. There is
also a risk that certain adverse events may not be observed in clinical trials, but may nonetheless occur in the future. If any
of these adverse events occur, they may render LO2A ineffective or harmful in some patients, and our sales would suffer, materially
adversely affecting our business, financial condition and results of operations.
The clinical trials we carry out are with
an insurance policy that allows the trials to be conducted. Accordingly, it is uncertain whether we will be able to complete our
receipt of the regulatory approvals for marketing the drug. Furthermore, it is uncertain whether indemnification will be provided
by the insurance companies. In addition, potential adverse events caused by LO2A could lead to product liability lawsuits. If product
liability lawsuits are successfully brought against us, we may incur substantial liabilities and may be required to limit the marketing
and commercialization of LO2A. Our business is exposed to potential product liability risks, which are inherent in the testing,
manufacturing, marketing and sale of pharmaceutical products. We may not be able to avoid product liability claims. Product liability
insurance for the pharmaceutical and biotechnology industries is generally expensive, if available at all. If, at any time, we
are unable to obtain sufficient insurance coverage on reasonable terms or to otherwise protect against potential product liability
claims, we may be unable to clinically test, market or commercialize LO2A. A successful product liability claim brought against
us in excess of our insurance coverage, if any, may cause us to incur substantial liabilities, and, as a result, our business,
liquidity and results of operations would be materially adversely affected.
LO2A will remain subject to ongoing
regulatory requirements even if it receives marketing approval, and if we fail to comply with these requirements, we could lose
these approvals, and the sales of any approved commercial products could be suspended.
Even if we receive regulatory approval to
market LO2A, the product will remain subject to extensive regulatory requirements, including requirements relating to manufacturing,
labeling, packaging, adverse event reporting, storage, advertising, promotion, distribution and recordkeeping. Even if regulatory
approval of a product is granted, the approval may be subject to limitations on the uses for which the product may be marketed
or the conditions of approval, or may contain requirements for costly post-marketing testing and surveillance to monitor the safety
or efficacy of the product, which could negatively impact us or our collaboration partners by reducing revenues or increasing expenses,
and cause the approved product candidate not to be commercially viable. In addition, as clinical experience with a drug expands
after approval, typically because it is used by a greater number and more diverse group of patients after approval than during
clinical trials, side effects and other problems may be observed after approval that were not seen or anticipated during pre-approval
clinical trials or other studies. Any adverse effects observed after the approval and marketing of a product candidate could result
in limitations on the use of or withdrawal of any approved products from the marketplace. Absence of long-term safety data may
also limit the approved uses of our products, if any. If we fail to comply with the regulatory requirements of the FDA and other
applicable U.S. and foreign regulatory authorities, or previously unknown problems with any approved commercial products, manufacturers
or manufacturing processes are discovered, we could be subject to administrative or judicially imposed sanctions or other setbacks,
including the following:
||restrictions on the products, manufacturers or manufacturing process;|
||civil or criminal penalties, fines and injunctions;|
||product seizures or detentions;|
||import or export bans or restrictions;|
||voluntary or mandatory product recalls and related publicity requirements;|
||suspension or withdrawal of regulatory approvals;|
||total or partial suspension of production; and|
||refusal to approve pending applications for marketing approval of new products or supplements to approved applications.|
If we or our collaborators are slow or unable
to adapt to changes in existing regulatory requirements or adoption of new regulatory requirements or policies, marketing approval
for LO2A may be lost or cease to be achievable, resulting in decreased revenue from milestones, product sales or royalties, which
would have a material adverse effect on our results of operations.
We rely significantly on information
technology and any failure, inadequacy, interruption or security lapse of that technology, including any cybersecurity incidents,
could harm our ability to operate our business effectively.
Despite the implementation of security measures,
our internal computer systems and those of third parties with which we contract are vulnerable to damage from cyber-attacks, computer
viruses, unauthorized access, natural disasters, terrorism, war and telecommunication and electrical failures. System failures,
accidents or security breaches could cause interruptions in our operations, and could result in a material disruption of our clinical
activities and business operations, in addition to possibly requiring substantial expenditures of resources to remedy. The loss
of clinical trial data could result in delays in our regulatory approval efforts and significantly increase our costs to recover
or reproduce the data. To the extent that any disruption or security breach were to result in a loss of, or damage to, our data
or applications, or inappropriate disclosure of confidential or proprietary information, we could incur liability and our research
and development programs and the development of LO2A could be delayed.
We may encounter difficulties in managing
our growth. Failure to manage our growth effectively will have a material adverse effect on our business, results of operations
and financial condition.
We may not be able to successfully grow
and expand. Successful implementation of our business plan will require management of growth, including potentially rapid and substantial
growth, which will result in an increase in the level of responsibility for management personnel and place a strain on our human
and capital resources. To manage growth effectively, we will be required to continue to implement and improve our operating and
financial systems and controls to expand, train and manage our employee base. Our ability to manage our operations and growth effectively
requires us to continue to expend funds to enhance our operational, financial and management controls, reporting systems and procedures
and to attract and retain sufficient numbers of talented personnel. If we are unable to scale up and implement improvements to
our control systems in an efficient or timely manner, or if we encounter deficiencies in existing systems and controls, then we
will not be able to make available the products required to successfully commercialize our technology. Failure to attract and retain
sufficient numbers of talented personnel will further strain our human resources and could impede our growth or result in ineffective
growth. Moreover, the management, systems and controls currently in place or to be implemented may not be adequate for such growth,
and the steps taken to hire personnel and to improve such systems and controls might not be sufficient. If we are unable to manage
our growth effectively, it will have a material adverse effect on our business, results of operations and financial condition.
If we are unable to obtain adequate
insurance, our financial condition could be adversely affected in the event of uninsured or inadequately insured loss or damage.
Our ability to effectively recruit and retain qualified officers and directors could also be adversely affected if we experience
difficulty in obtaining adequate directors’ and officers’ liability insurance.
We may not be able to obtain insurance policies
on terms affordable that would adequately insure our business and property against damage, loss or claims by third parties. To
the extent our business or property suffers any damages, losses or claims by third parties, which are not covered or adequately
covered by insurance, our financial condition may be materially adversely affected.
We may be unable to maintain sufficient
insurance as a public company to cover liability claims made against our officers and directors. If we are unable to adequately
insure our officers and directors, we may not be able to retain or recruit qualified officers and directors to manage our business.
Risks Related to our Intellectual Property
Our ability to pursue the purchase,
marketing, sale and distribution of LO2A depends upon the continuation of the LO2A License Agreement.
We do not own LO2A. We have entered
into the LO2A License Agreement with Resdevco to license certain rights to LO2A (see Item 1 - “BUSINESS
— LO2A License Agreement,” beginning on page 8 of this Annual Report). The LO2A License Agreement requires
us to, among other things, make certain minimum royalty payments to Resdevco and meet certain regulatory milestones. If we do
not meet our obligations under the LO2A License Agreement in a timely manner, or if we otherwise breach the terms of the LO2A
License Agreement, Resdevco could terminate the LO2A License Agreement and we would lose the rights to LO2A. From time to
time, in the ordinary course of business, we may have disagreements with Resdevco regarding the terms of the LO2A License
Agreement or ownership of proprietary rights, which could lead to delays in the research, development, collaboration and
commercialization of LO2A, or could require or result in litigation or arbitration, which could be time-consuming and
expensive. If the LO2A License Agreement is terminated, it would have a material adverse effect on our business, prospects
and results of operations.
Our inability to expand our rights
under the LO2A License Agreement may have a detrimental effect on our business.
Pursuant to the LO2A License Agreement,
we have (i) the right to add additional territories in the future, subject to a commitment by us to pay minimum royalties, (ii)
the right to purchase Resdevco’s agreements with its existing distributors of LO2A in other jurisdictions, subject to the
payment by us of the amount set forth in the LO2A License Agreement, and (iii) a right of first negotiation with potential distributors
to whom Resdevco may in the future grant distribution rights to LO2A in certain territories, subject to the payment by us of certain
minimum royalties. The LO2A License Agreement historically included an option for us to purchase from Resdevco all remaining territories
for a fixed amount and such option was cancelled on March 30, 2017.
Our ability to exercise our rights mentioned
above and to expand our business is subject to us having sufficient cash resources to make the applicable payments to Resdevco.
If we do not have sufficient cash resources to make such payments, we will not be able to exercise our expansion rights under the
LO2A License Agreement and our business may suffer.
The failure to obtain or maintain
patents and other intellectual property could impact our ability to compete effectively.
Our success, competitive position, and future
revenues, if any, depend in part on our ability to obtain and successfully leverage intellectual property covering LO2A, know-how,
methods, processes, and other technologies, to protect our trade secrets, to prevent others from using our intellectual property
and to operate without infringing the intellectual property rights of third parties.
The risks and uncertainties that we face
with respect to our intellectual property rights include, but are not limited to, the following:
||while any patents that we license under the LO2A License Agreement have been issued, their scope of protection is limited to the CCH indication in the United States;|
||we may not obtain rights from Resdevco to any further patents or patent applications related to LO2A;|
||we or Resdevco may be subject to interference proceedings;|
||we or Resdevco may be subject to opposition proceedings in foreign countries;|
||any patent that is issued may not provide meaningful protection;|
||we or Resdevco may not be able to develop additional proprietary technologies that are patentable;|
||other companies may challenge patents licensed or issued to us or our customers;|
||other companies may independently develop similar or alternative technologies, or duplicate our technologies;|
||other companies may design around technologies we have licensed or developed; and|
||enforcement of patents is complex, uncertain and expensive.|
If patent rights covering LO2A are not sufficiently
broad or expire, they may not provide us with any protection against competitors with similar products and technologies. For example,
a patent covering the composition and use of LO2A for treating or alleviating DES has expired. Furthermore, if the United
States Patent and Trademark Office (the “USPTO”), or foreign patent offices issue patents to us or our licensors, others
may challenge the patents or design around the patents, or the patent office or the courts may invalidate the patents. Thus,
any patents we own or license from or to third parties may not provide any protection against our competitors.
We cannot be certain that patents will be
issued as a result of any pending applications, and cannot be certain that any of our issued patents, including those licensed
from Resdevco or any other third-party in the future, will give us adequate protection from competing products. For example, issued
patents, including the patents licensed by us, may be circumvented or challenged, declared invalid or unenforceable, or narrowed
In addition, since publication of discoveries
in the scientific or patent literature often lags behind actual discoveries, we cannot be certain that we or Resdevco were or will
be the first to make our inventions or to file patent applications covering those inventions.
It is also possible that others may obtain
issued patents that could prevent us from commercializing LO2A or require us to obtain licenses requiring the payment of significant
fees or royalties in order to enable us to conduct our business. As to those patents that we have licensed, our rights depend on
maintaining our obligations to the licensor under the applicable license agreement, and we may be unable to do so.
In addition to patents and patent applications,
we depend upon trade secrets and proprietary know-how to protect our proprietary technology. We require our employees, consultants,
advisors and collaborators to enter into confidentiality agreements that prohibit the disclosure of confidential information to
any other parties. We require our employees and consultants to disclose and assign their ideas, developments, discoveries and inventions
to us. These agreements may not, however, provide adequate protection for our trade secrets, know-how or other proprietary information
in the event of any unauthorized use or disclosure.
Costly litigation may be necessary
to protect our or Resdevco’s intellectual property rights and we or Resdevco may be subject to claims alleging the violation
of the intellectual property rights of others.
Our activity in the field of life sciences
exposes us to the possibility of legal proceedings connected with our business activities. We may face significant expense and
liability as a result of litigation or other proceedings relating to patents and other intellectual property rights of others.
In the event that another party has also filed a patent application or been issued a patent relating to an invention or technology
claimed by us or Resdevco in pending applications, we may be required to participate in an interference proceeding declared by
the USPTO to determine priority of invention, which could result in substantial uncertainties and costs for us, even if the eventual
outcome was favorable to us. We, or our licensors, could be required to participate in interference proceedings involving issued
patents and pending applications of another entity. An adverse outcome in an interference proceeding could require us to cease
using the technology or to license rights from prevailing third parties.
The cost to us of any patent litigation
or other proceeding relating to our licensed patents or patent applications, even if resolved in our favor, could be substantial.
The ability of us and Resdevco to enforce our patent protection could be limited by our financial resources, and may be subject
to lengthy delays. If we are unable to effectively enforce our or Resdevco’s proprietary rights, or if we are found to infringe
the rights of others, we may be in breach of the LO2A License Agreement.
A third party may claim that we or Resdevco
are using inventions claimed by their patents and may go to court to stop us or Resdevco from engaging in our normal operations
and activities, such as research, development and the sale of any future products. Such lawsuits are expensive and would consume
time and other resources. There is a risk that the court will decide that we or Resdevco are infringing the third party’s
patents and will order us or Resdevco to stop the activities claimed by the patents, redesign our products or processes to avoid
infringement or obtain licenses (which may not be available on commercially reasonable terms). In addition, there is a risk that
a court will order us to pay the other party damages for having infringed their patents.
Moreover, there is no guarantee that any
prevailing patent owner would offer us or Resdevco a license so that we or Resdevco could continue to engage in activities claimed
by the patent, or that such a license, if made available, could be acquired on commercially acceptable terms. In addition, third
parties may, in the future, assert other intellectual property infringement claims against us or Resdevco with respect to its product
candidates, technologies or other matters.
We rely on our and Resdevco’s
confidentiality agreements that could be breached and may be difficult to enforce, which could result in third parties using our
intellectual property to compete against us.
Although we believe that we take reasonable
steps to protect our intellectual property, including the use of agreements relating to the non-disclosure of confidential information
to third parties, as well as agreements that purport to require the disclosure and assignment of the rights to the ideas, developments,
discoveries and inventions of our employees and consultants while they are employed by us and we believe that Resdevco also takes
such measures, the agreements can be difficult and costly to enforce. Although we believe that our licensors seek to obtain these
types of agreements from our contractors, consultants, advisors and research collaborators, to the extent that employees and consultants
utilize or independently develop intellectual property in connection with any of our projects, disputes may arise as to the intellectual
property rights associated with our products. If a dispute arises, a court may determine that the right belongs to a third party.
In addition, enforcement of our and Resdevco’s rights can be costly and unpredictable. We and Resdevco also rely on trade
secrets and proprietary know-how that we believe that Resdevco seeks to protect in part by confidentiality agreements with employees,
contractors, consultants, advisors or others. Despite the protective measures we and Resdevco employ, we still face the risk that:
||these agreements may be breached;|
||these agreements may not provide adequate remedies for the applicable type of breach;|
||our and Resdevco’s trade secrets or proprietary know-how will otherwise become known; or|
||our competitors will independently develop similar technology or proprietary information.|
Patent protection outside the United
States is particularly uncertain, and if we are involved in opposition proceedings outside the United States, we may have to expend
substantial sums and management resources.
Patent law outside the United States is
different than in the United States. Further, the laws of some foreign countries may not protect our or Resdevco’s intellectual
property rights to the same extent as the laws of the United States, if at all. A failure to obtain sufficient intellectual
property protection in any country could materially and adversely affect our business, results of operations and future prospects.
Moreover, we may participate in opposition proceedings to determine the validity of our foreign patents or our competitors’
foreign patents, which could result in substantial costs and divert management’s resources and attention.
We may not be able to enforce employees’
and consultants covenants not to compete and therefore may be unable to prevent our competitors from benefiting from the expertise
of some of our former employees or consultants.
We have entered into non-competition agreements
with our key employees and key consultants, within the framework of their employment agreements or consultant agreements, respectively.
These agreements prohibit such persons, if they cease working for us, from competing directly with us or working for our competitors
for a limited period. Under applicable law, we may be unable to enforce these agreements. If we cannot enforce our non-competition
agreements with such persons, then we may be unable to prevent our competitors from benefiting from the expertise of our former
employees and consultants, which could materially adversely affect our business, results of operations and ability to capitalize
on our proprietary information.
Intellectual property rights do not
necessarily address all potential threats to our competitive advantage.
The degree of future protection afforded
by our intellectual property rights is uncertain because intellectual property rights have limitations, and may not adequately
protect our business, or permit us to maintain our competitive advantage. The following examples are illustrative:
||Others may be able to make compounds that are the same as or similar to LO2A but that are not covered by the claims of the patents that we have exclusively licensed;|
||Resdevco or any future strategic partners might not have been the first to make the inventions covered by the issued patent or pending patent applications that we have exclusively licensed;|
||Resdevco or any future strategic partners might not have been the first to file patent applications covering certain of our technology;|
||Others may independently develop similar or alternative technologies or duplicate any of our technologies without infringing our intellectual property rights;|
||It is possible that any pending patent applications will not lead to issued patents;|
||Issued patents that we have exclusively licensed may not provide us with any competitive advantages, or may be held invalid or unenforceable, as a result of legal challenges by our competitors;|
||Our competitors might conduct research and development activities in countries where we do not have patent rights and then use the information learned from such activities to develop competitive products for sale in our major commercial markets; |
||We may not develop additional proprietary technologies that are patentable; and |
||The patents of others may have an adverse effect on our business. |
We may be subject to claims challenging
the inventorship of our patents and other intellectual property.
We may be subject to claims that former
employees, collaborators or other third parties have an interest in our patents or other intellectual property as an inventor or
co-inventor. For example, we may have inventorship disputes arise from conflicting obligations of consultants or others who are
involved in developing our product candidates. Litigation may be necessary to defend against these and other claims challenging
inventorship. If we fail in defending any such claims, in addition to paying monetary damages, we may lose valuable intellectual
property rights, such as exclusive ownership of, or right to use, valuable intellectual property. Such an outcome could have a
material adverse effect on our business. Even if we are successful in defending against such claims, litigation could result in
substantial costs and be a distraction to management and other employees.
Risks Related to our Industry
We are subject to government regulations
and we may experience delays in obtaining required regulatory approvals to market LO2A.
Various aspects of our operations are subject
to federal, state or local laws, rules and regulations, any of which may change from time to time. Costs arising out of any regulatory
developments could be time-consuming and expensive and could divert management resources and attention and, consequently, could
adversely affect our business operations and financial performance.
Delays in regulatory approval, limitations
in regulatory approval and withdrawals of regulatory approval may have a material adverse effect on us. If we experience significant
delays in testing or receiving approvals or sign-offs to conduct clinical trials, our product development costs, or our ability
to license LO2A, will increase. If certain country’s regulatory authority grants regulatory approval to market a product,
this approval will be limited to those disease states and conditions for which the product has demonstrated, through clinical trials,
to be safe and effective. Any product approvals that we receive in the future could also include significant restrictions on the
use or marketing of our products. Product approvals, if granted, can be withdrawn for failure to comply with regulatory requirements
or upon the occurrence of adverse events following commercial introduction of the products. Failure to comply with applicable regulatory
requirements may result in criminal prosecution, civil penalties, recall or seizure of products, total or partial suspension of
production or injunction, as well as other regulatory action against us or LO2A. If approval is withdrawn for a product, or if
a product were seized or recalled, we would be unable to sell or license that product and our revenues would suffer.
We expect the healthcare industry
to face increased limitations on reimbursement as a result of healthcare reform, which could adversely affect third-party coverage
of our products and how much or under what circumstances healthcare providers will prescribe or administer our products.
In both the United States and other countries,
sales of our products will depend in part upon the availability of reimbursement from third-party payors, which include governmental
authorities, managed care organizations and other private health insurers. Third-party payors are increasingly challenging the
price and examining the cost effectiveness of medical products and services.
Increasing expenditures for healthcare have
been the subject of considerable public attention in the United States. Both private and government entities are seeking ways to
reduce or contain healthcare costs. Numerous proposals that would effect changes in the U.S. healthcare system have been introduced
or proposed in Congress and in some state legislatures, including reducing reimbursement for prescription products and reducing
the levels at which consumers and healthcare providers are reimbursed for purchases of pharmaceutical products.
In 2010, the United States Congress enacted
the Patient Protection and Affordable Care Act of 2010 or, Affordable Care Act. The Affordable Care Act seeks to reduce the federal
deficit and the rate of growth in health care spending through, among other things, stronger prevention and wellness measures,
increased access to primary care, changes in health care delivery systems and the creation of health insurance exchanges. Enrollment
in the health insurance exchanges began in October 2013. The Affordable Care Act requires the pharmaceutical industry to share
in the costs of reform, by, among other things, increasing Medicaid rebates and expanding Medicaid rebates to cover Medicaid managed
care programs. Other components of healthcare reform include funding of pharmaceutical costs for Medicare patients in excess of
the prescription drug coverage limit and below the catastrophic coverage threshold. Under the Affordable Care Act, pharmaceutical
companies are now obligated to fund 50% of the patient obligation for branded prescription pharmaceuticals in this gap, or “donut
hole.” Additionally, commencing in 2011, an excise tax was levied against certain branded pharmaceutical products. The tax
is specified by statute to be approximately $3 billion in 2012 through 2016, $3.5 billion in 2017, $4.2 billion in 2018, and $2.8
billion each year thereafter. The tax is to be apportioned to qualifying pharmaceutical companies based on an allocation of their
governmental programs as a portion of total pharmaceutical government programs.
Although we cannot predict the full effect
on our business of the implementation of existing legislation, including the Affordable Care Act or the enactment of additional
legislation, we believe that legislation or regulations that reduce reimbursement for or restrict coverage of our products could
adversely affect how much or under what circumstances healthcare providers will prescribe or administer our products. This could
materially and adversely affect our business by reducing our ability to generate revenue, raise capital, obtain additional collaborators
and market our products. In addition, we believe the increasing emphasis on managed care in the United States has and will continue
to put pressure on the price and usage of pharmaceutical products, which may adversely impact product sales.
We may be subject to U.S. and foreign
anti-kickback laws and regulations. Our failure to comply with these laws and regulations could have adverse consequences.
There are extensive U.S. federal and state
laws and regulations prohibiting fraud and abuse in the healthcare industry that can result in significant criminal and civil penalties.
These federal laws include: the anti-kickback statute, which prohibits certain business practices and relationships, including
the payment or receipt of remuneration for the referral of patients whose care will be paid by Medicare or other federal healthcare
programs; the physician self-referral prohibition, commonly referred to as the Stark Law; the anti-inducement law, which prohibits
providers from offering anything to a Medicare or Medicaid beneficiary to induce that beneficiary to use items or services covered
by either program; the False Claims Act, which prohibits any person from knowingly presenting or causing to be presented false
or fraudulent claims for payment by the federal government, including the Medicare and Medicaid programs; and the Civil Monetary
Penalties Law, which authorizes the U.S. Department of Health and Human Services to impose civil penalties administratively for
fraudulent or abusive acts.
for violating these federal laws include criminal and civil penalties that range from punitive sanctions, damage assessments,
money penalties, imprisonment, denial of Medicare and Medicaid payments, or exclusion from the Medicare and Medicaid programs,
or both, and debarment. As federal and state budget pressures continue, federal and state administrative agencies may also continue
to escalate investigation and enforcement efforts to root out waste and to control fraud and abuse in governmental healthcare
programs. Private enforcement of healthcare fraud has also increased, due in large part to amendments to the civil False Claims
Act in 1986 that were designed to encourage private persons to sue on behalf of the government. A violation of any of these federal
and state fraud and abuse laws and regulations or any similar law in a different jurisdiction which is applicable to us could
have a material adverse effect on our liquidity and financial condition. An investigation into the use by physicians of any of
our products once commercialized may dissuade physicians from either purchasing or using them, and could have a material adverse
effect on our ability to commercialize those products.
Related to Our Common Stock
failure of our business to succeed may result in the depression in the value of our Common Stock.
LO2A is approved for sale in certain jurisdictions for the treatment of DES, LO2A is only approved for sale for the treatment
of CCH in Hungary and for the treatment of Sjögren’s in the Netherlands. LO2A may never be successfully developed and
approved for sale or successfully commercialized for the treatment of CCH or for Sjögren’s in any other jurisdiction.
The failure to successfully commercialize LO2A for the treatment of CCH and Sjögren’s may have a material adverse effect
on our business and could depress the value of our Common Stock.
restricted shares are subject to resale restrictions imposed by Rule 144, including those set forth in Rule 144(i) which applies
to a “shell company.”
to the Merger, we were a “shell company” under applicable SEC rules and regulations. Pursuant to Rule 144, promulgated
under the Securities Act, sales of the securities of a shell company, such as ours under that rule are not permitted until at
least 12 months have elapsed from the date on which we file with the SEC Form 10 information in a Current Report on Form 8-K,
reflecting our status as a non-shell company (which occurred on November 21, 2017). As a result, some of our stockholders
would be forced to hold their shares of Common Stock for at least that 12-month period before they are eligible to sell those
shares, and even after that 12-month period, sales may not be made under Rule 144 unless we and our relevant stockholders are
in compliance with other requirements of Rule 144. Further, it will be more difficult for us to raise funding to support
our operations through the sale of debt or equity securities, unless we agree to register such securities under the Securities
Act, which could cause us to expend additional time and cash resources. The lack of liquidity of our securities as a result
of the inability to sell under Rule 144 for a longer period of time could cause the market price of our securities to decline.
large number of shares are issuable upon exercise of outstanding Convertible Loans, Investment Rights or PIPE Warrants. The exercise
of these securities could result in the substantial dilution of your investment in terms of your percentage ownership in our company.
The sale of a large amount of Common Stock received upon exercise of these securities on the public market, or the perception
that such sales could occur, could substantially depress the prevailing market prices for our shares.
of March 28, 2018, there were outstanding presently exercisable (i) Convertible Loans entitling the holders to purchase 1,355,775
shares of Common Stock at a weighted average exercise price of $1.0536 per share, (ii) Investment Rights entitling the holders
to purchase 1,103,662 shares of Common Stock at a weighted average exercise price of $1.3224 per share, and (iii) PIPE Warrants
entitling the holders to purchase 759,869 shares of Common Stock at a weighted average exercise price of $1.9728 per share. The
exercise or conversion price for all of the aforesaid securities may be less than your cost to acquire our shares. In the event
of the exercise or conversion of these securities, you could suffer substantial dilution of your investment in terms of your percentage
ownership in our company. In addition, the holders of such securities may sell shares in tandem with their exercise of those securities
to finance that exercise, which could further depress the market price of the Common Stock.
additional capital may cause dilution to our existing stockholders, restrict our operations or require us to relinquish rights
may seek additional capital through a combination of private and public equity offerings, debt financings, strategic partnerships
and alliances and licensing arrangements. To the extent that we raise additional capital through the sale of equity or convertible
debt securities, the ownership interests of existing stockholders will be diluted, and the terms may include liquidation or other
preferences that adversely affect stockholder rights. Furthermore, the number of shares available for future grant under our equity
compensation plans may be increased in the future. Debt financing, if available, may involve agreements that include covenants
limiting or restricting our ability to take certain actions, such as incurring debt, making capital expenditures or declaring
dividends. If we raise additional funds through strategic partnerships and alliances and licensing arrangements with third parties,
we may have to relinquish valuable rights to our LO2A, or grant licenses on terms that are not favorable. If we are unable to
raise additional funds through equity or debt financing when needed, we may be required to delay, limit, reduce or terminate our
product development or commercialization efforts or grant rights to develop and market LO2A that we would otherwise prefer to
develop and market ourselves.
our Common Stock may be a “penny stock,” it may be more difficult for investors to sell shares of our Common Stock,
and the market price of our Common Stock may be adversely affected.
Common Stock may be a “penny stock” if, among other things, the stock price is below $5.00 per share, it is not listed
on a national securities exchange or it has not met certain net tangible asset or average revenue requirements. Broker-dealers
who sell penny stocks must provide purchasers of these stocks with a standardized risk-disclosure document prepared by the SEC.
This document provides information about penny stocks and the nature and level of risks involved in investing in the penny-stock
market. A broker must also give a purchaser, orally or in writing, bid and offer quotations and information regarding broker and
salesperson compensation, make a written determination that the penny stock is a suitable investment for the purchaser, and obtain
the purchaser’s written agreement to the purchase. Broker-dealers must also provide customers that hold penny stock in their
accounts with such broker-dealer a monthly statement containing price and market information relating to the penny stock. If
a penny stock is sold to an investor in violation of the penny stock rules, the investor may be able to cancel its purchase and
get its money back.
applicable, the penny stock rules may make it difficult for investors to sell our shares of Common Stock. Because of the
rules and restrictions applicable to a penny stock, there is less trading in penny stocks and the market price of our Common Stock
may be adversely affected. Also, many brokers choose not to participate in penny stock transactions. Accordingly, investors
may not always be able to resell their shares of our Common Stock publicly at times and prices that they feel are appropriate.
may not be able to attract the attention of major brokerage firms, which may limit the liquidity of our Common Stock and may make
it more difficult for us to raise additional capital in the future.
analysts of major brokerage firms may not provide coverage of our Common Stock because there may be little incentive for brokerage
firms to recommend the purchase of our Common Stock. As a result, our Common Stock may have limited liquidity and investors may
have difficulty selling it. Furthermore, we cannot assure you that brokerage firms will want to conduct any secondary
offerings on our behalf if we seek to raise additional capital in the future. Our inability to raise additional capital
may have a material adverse effect on our business.
sales of our Common Stock could reduce our stock price.
by stockholders of substantial amounts of our Common Stock, or the perception that these sales may occur in the future, including
the sale of shares by certain stockholders upon the expiration of the tax withholding deferral period set forth in the 104(h)
Tax Ruling, could materially and adversely affect the market price of our Common Stock. Furthermore, the market price of our Common
Stock could drop significantly if our executive officers, directors, or certain large shareholders sell their shares, or are perceived
by the market as intending to sell them.
concentration of the capital stock ownership with our insiders will likely limit the ability of our stockholders to influence
of March 28, 2018, our executive officers, directors, five percent or greater stockholders, and their respective affiliated entities
in the aggregate beneficially own approximately 86% of our Common Stock. As a result of such ownership, despite the fact that
each one of them, to our knowledge, will continue to operate independently from the other with respect to their respective shareholding
of the Company’s shares, these stockholders, if acting together, will have control over matters that require approval by
our stockholders, including the election of directors and approval of significant corporate transactions. Corporate actions might
be taken even if other stockholders oppose them. This concentration of ownership might also have the effect of delaying or preventing
a corporate transaction that other stockholders may view as beneficial, including preventing changes in control or in management.
For more information about our current share ownership, please see Item 12 - “SECURITY OWNERSHIP OF CERTAIN BENEFICIAL OWNERS
AND MANAGEMENT AND RELATED STOCKHOLDER MATTERS,” beginning on page 82 of this Annual Report.
may not be able to timely and effectively implement controls and procedures required by Section 404 of the Sarbanes-Oxley Act
to the Merger, Wize Israel was traded on the Tel Aviv Stock Exchange (“TASE”) and was not subject to Section 404 of
the Sarbanes-Oxley Act of 2002. The standards required for a public company under Section 404 of the Sarbanes-Oxley Act of 2002
are different from those required of a public company whose shares are traded on the TASE. Management may not be able to effectively
and timely implement controls and procedures that adequately respond to the regulatory compliance and reporting requirements that
are applicable to us after the Merger. If management is not able to implement the additional requirements of Section 404 of the
Sarbanes-Oxley Act of 2002 in a timely manner or with adequate compliance, it may not be able to assess whether its internal control
over financial reporting is effective, which may subject us to adverse regulatory consequences and could harm investor confidence
and the market price of our Common Stock.
a result of the Merger, we may be required to take restructuring or other charges that could have a significant negative effect
on our financial condition, results of operations and stock price, which could cause you to lose some or all of your investment.
a result of the Merger, the liabilities of Wize Israel, our wholly owned Israeli subsidiary, including contingent liabilities,
were consolidated into our financial statements. Although both parties conducted due diligence on each other, there can be no
assurances that the diligence revealed all material issues that may be present in the other company’s business, that all
material issues through a customary amount of due diligence will be uncovered, or that factors outside of our control will not
later arise. As a result, we may be forced to later restructure operations, or other charges that could result in losses. Even
if due diligence successfully identifies certain risks, unexpected risks may arise and previously known risks may materialize
in a manner not consistent with each company’s preliminary risk analysis. Even though these charges may be non-cash items
and not have an immediate impact on liquidity, the fact that we report charges of this nature could contribute to negative market
perceptions about us or our securities. In addition, charges of this nature may make future financing difficult to obtain on favorable
terms or at all. If unknown pre-Merger liabilities arise, we may be required to divert cash from other business purposes to discharge
such liabilities, which may have an adverse effect on our business.
an “emerging growth company” under the JOBS Act, we are permitted to, and intend to, rely on exemptions from certain
an “emerging growth company” under the JOBS Act, we are permitted to, and intend to, rely on exemptions from certain
disclosure requirements. We are an emerging growth company until the earliest of: (i) the last day of the fiscal year during
which hawse have total annual gross revenues of $1 billion or more, (ii) the last day of the fiscal year following the fifth anniversary
of the date of the first sale of our Common Stock pursuant to an effective registration statement, (iii) the date on which we
have, during the previous three-year period, issued more than $1 billion in non-convertible debt or (iv) the date on which we
are deemed a “large accelerated issuer” as defined in Regulation S-K of the Securities Act. For so long as we
remain an emerging growth company, we will not be required to:
an auditor report on our internal control over financial reporting pursuant to Section 404(b) of the Sarbanes-Oxley Act;|
with any requirement that may be adopted by the Public Company Accounting Oversight Board regarding mandatory audit firm rotation
or a supplement to the auditor’s report providing additional information about the audit and the financial statements
(auditor discussion and analysis);|
certain executive compensation matters to stockholders advisory votes pursuant to the “say on frequency” and “say
on pay” provisions (requiring a non-binding stockholder vote to approve compensation of certain executive officers)
and the “say on golden parachute” provisions (requiring a non-binding stockholder vote to approve golden parachute
arrangements for certain executive officers in connection with mergers and certain other business combinations) of the Dodd-Frank
Wall Street Reform and Consumer Protection Act of 2010; and|
detailed compensation discussion and analysis in its filings under the Exchange Act, and instead may provide a reduced level
of disclosure concerning executive compensation. |
we intend to rely on the exemptions provided in the JOBS Act, the exact implications of the JOBS Act are still subject to interpretations
and guidance by the SEC and other regulatory agencies. In addition, as our business grows, we may no longer satisfy the
conditions of an emerging growth company.
have not paid, and do not intend to pay, dividends on our Common Stock and therefore, unless our Common Stock appreciates in value,
our investors may not benefit from holding our Common Stock.
have not paid any cash dividends on our Common Stock since inception and do not anticipate paying any cash dividends on our Common
Stock in the foreseeable future. In addition, we are restricted from paying any dividends without Rimon Gold’s consent
so long as our loans from Rimon Gold have not been repaid in full. As a result, investors in our Common Stock will not be able
to benefit from owning our Common Stock unless the market price of our Common Stock becomes greater than the price paid for the
stock by these investors.
provisions under Delaware law could make an acquisition of us, which may be beneficial to our stockholders, more difficult and
may prevent attempts by the stockholders to replace or remove management.
will be subject to the anti-takeover provisions of the Delaware General Corporation Law (“DGCL”), including Section
203. Under these provisions, if anyone becomes an “interested stockholder,” the combined company may not enter into
a “business combination” with that person for three years without special approval, which could discourage a third
party from making a takeover offer and could delay or prevent a change of control. For purposes of Section 203 of the DGCL, “interested
stockholder” means, generally, someone owning 15% or more of the combined company’s outstanding voting stock or an
affiliate of the combined company that owned 15% or more of the combined company’s outstanding voting stock during the past
three years, subject to certain exceptions as described in Section 203 of the DGCL. In addition, our Certificate of Incorporation
contains provisions, such as blank check preferred stock, advance notice, and stockholder action by written consent which could
make it more difficult for a third party to acquire us. These provisions may have the effect of preventing or hindering any attempts
by our stockholders to replace our Board of Directors or management.
public trading market for our Common Stock is volatile and may result in higher spreads in stock prices, which may limit the ability
of our investors to sell their shares at a profit, if at all.
Common Stock trades in the over-the-counter market and is quoted on the OTCQB. The over-the-counter market for securities
has historically experienced extreme price and volume fluctuations during certain periods. These broad market fluctuations
may adversely affect the market price of our Common Stock and result in substantial losses to its investors. In addition, the
spreads on stock traded through the over-the-counter market are generally unregulated and higher than on stock exchanges, which
mean that the difference between the price at which shares could be purchased by investors in the over-the-counter market compared
to the price at which they could be subsequently sold would be greater than on these exchanges. Significant spreads between
the bid and asked prices of the stock could continue during any period in which a sufficient volume of trading is unavailable
or if the stock is quoted by an insignificant number of market makers. Historically our trading volume has been insufficient
to significantly reduce this spread and has had a limited number of market makers sufficient to affect this spread. These
higher spreads could adversely affect investors who purchase the shares at the higher price at which the shares are sold, but
subsequently sell the shares at the lower bid prices quoted by the brokers. Unless the bid price for the stock exceeds the
price paid for the shares by the investor, plus brokerage commissions or charges, the investor could lose money on the sale. For
higher spreads such as those on over-the-counter stocks, this is likely a much greater percentage of the price of the stock than
for exchange listed stocks. There is no assurance that at the time an investor in our Common Stock wishes to sell the shares,
the bid price will have sufficiently increased to create a profit on the sale.
active market for our Common Stock may not develop.
our Common Stock trades on the OTCQB, we do not have an active trading market and an active trading market may not develop. If
an active trading market does not develop, or is not sustained, it may be difficult for investors to sell their shares without
depressing the market price for the shares or at all. Further, an inactive market may also impair our ability to raise capital
by selling shares of our Common Stock and may impair our ability to enter into strategic partnerships or acquire companies or
products by using our shares of Common Stock as consideration.
Common Stock is thinly traded, so you may be unable to sell at or near ask prices or at all if you need to sell your shares to
raise money or otherwise desire to liquidate your shares.
Common Stock has historically been sporadically traded on the OTCQB, meaning that the number of persons interested in purchasing
our shares at or near ask prices at any given time may be relatively small or non-existent. This situation is attributable to
a number of factors, including the fact that we are a small company which is relatively unknown to stock analysts, stock brokers,
institutional investors and others in the investment community that generate or influence sales volume, and that even if we came
to the attention of such persons, they tend to be risk-averse and would be reluctant to follow an unproven company such as ours
or purchase or recommend the purchase of our shares until such time as we became more seasoned and viable. As a consequence, there
may be periods of several days or more when trading activity in our shares is minimal or non-existent, as compared to a seasoned
issuer which has a large and steady volume of trading activity that will generally support continuous sales without an adverse
effect on share price. We cannot give you any assurance that a broader or more active public trading market for our Common Stock
will develop or be sustained, or that current trading levels will be sustained.
Board can, without stockholder approval, cause preferred stock to be issued on terms that adversely affect common stockholders
or which could be used to resist a potential take-over of us.
our Certificate of Incorporation, our Board is authorized to issue up to 1,000,000 shares of preferred stock, none of which are
issued and outstanding as of the date of this Annual Report. Also, our Board, without stockholder approval, may determine
the price, rights, preferences, privileges and restrictions, including voting rights, of those shares. If the Board causes
shares of preferred stock to be issued, the rights of the holders of our Common Stock could be adversely affected. The Board’s
ability to determine the terms of preferred stock and to cause its issuance, while providing desirable flexibility in connection
with possible acquisitions and other corporate purposes, could have the effect of making it more difficult for a third party to
acquire a majority of our outstanding voting stock. Preferred shares issued by the Board could include voting rights, or
even super voting rights, which could shift the ability to control us to the holders of the preferred stock. Preferred shares
could also have conversion rights into shares of Common Stock at a discount to the market price of the Common Stock which could
negatively affect the market for our Common Stock. In addition, preferred shares would have preference in the event of liquidation
of the corporation, which means that the holders of preferred shares would be entitled to receive the net assets of the corporation
distributed in liquidation before the Common Stock holders receive any distribution of the liquidated assets. We have no
current plans to issue any shares of preferred stock.
market price of our Common Stock may fluctuate significantly, which could result in substantial losses by our investors.
market price of our Common Stock may fluctuate significantly in response to numerous factors, some of which are beyond its control,
of technological innovations, new products or product enhancements by us or others;|
by us of significant strategic partnerships, out-licensing, in-licensing, joint ventures, acquisitions or capital commitments;|
or terminations of licenses, research contracts or other collaboration agreements;|
concern as to the safety of LO2A;|
of research and development projects;|
in clinical and preclinical studies;|
concerning intellectual property rights or regulatory approvals;|
in our and our competitors’ results of operations;|
in earnings estimates or recommendations by securities analysts, if our Common Stock is covered by analysts;|
in government regulations or patent decisions;|
by our licensees;|
in the biotechnology industry;|
results of product liability or intellectual property lawsuits;|
issuances of Common Stock or other securities;|
addition or departure of key personnel;|
by us or our competitors of acquisitions, investments or strategic alliances;|
market conditions, including the volatility of market prices for shares of biotechnology companies generally, and other factors,
including factors unrelated to our operating performance; and|
other factors described in Item 1A - “RISK FACTORS,” beginning on page 35 of this Annual Report. |
factors and any corresponding price fluctuations may materially and adversely affect the market price of our Common Stock and
result in substantial losses by our investors.
the stock market in general, and the market for biotechnology companies in particular, has experienced extreme price and volume
fluctuations in the past. Continued market fluctuations could result in extreme volatility in the price of our Common Stock,
which could cause a decline in the value of our Common Stock. Price volatility of our Common Stock might be worse if the
trading volume of our Common Stock is low. In the past, following periods of market volatility, stockholders have
often instituted securities class action litigation. If we are involved in securities litigation, it could have a substantial
cost and divert resources and attention of management from our business, even if successful. Future sales of our Common
Stock could also reduce the market price of such stock.
Related to our Operations in Israel
political, economic and military instability in the State of Israel, where our senior management and our head executive office
facilities are located, may adversely affect our results of operations.
executive office where we conduct initial research and development activities, as well as some of our clinical sites and suppliers
are located in Israel. Our officers and our directors are residents of Israel. Accordingly, political, economic and military
conditions in Israel and the surrounding region may directly affect our business and operations. Since the establishment
of the State of Israel in 1948, a number of armed conflicts have taken place between Israel and its Arab neighbors. Any hostilities
involving Israel or the interruption or curtailment of trade within Israel or between Israel and its trading partners could adversely
affect our operations and results of operations and could make it more difficult for us to raise capital. During the summer of
2014 and the winter of 2012 and 2008, Israel was engaged in an armed conflict with Hamas, a militia group and political party
operating in the Gaza Strip, and during the summer of 2006, Israel was engaged in an armed conflict with Hezbollah, a Lebanese
Islamist Shiite militia group and political party. These conflicts involved missile strikes against civilian targets in various
parts of Israel, and negatively affected business conditions in Israel. To date, Israel faces political tension with respect to
its relationships with Turkey, Iran and other Arab neighbor countries. In addition, recent political uprisings and social unrest
in various countries in the Middle East and North Africa are affecting the political stability of those countries. This instability
may lead to deterioration of the political relationships that exist between Israel and these countries, and have raised concerns
regarding security in the region and the potential for armed conflict. Any armed conflicts, terrorist activities or political
instability in the region could adversely affect business conditions and could harm our results of operations. For example, any
major escalation in hostilities in the region could result in a portion of our employees and service providers being called up
to perform military duty for an extended period of time. Parties with whom we do business have sometimes declined to travel to
Israel during periods of heightened unrest or tension, forcing us to make alternative arrangements when necessary. In addition,
the political and security situation in Israel may result in parties with whom we have agreements involving performance in Israel
claiming that they are not obligated to perform their commitments under those agreements pursuant to force majeure provisions
in such agreements. Any future deterioration in the political and security situation in Israel will negatively impact our business.
commercial insurance does not cover losses that may occur as a result of events associated with the security situation in the
Middle East. Although the Israeli government currently covers the reinstatement value of direct damages that are caused by terrorist
attacks or acts of war, we cannot assure you that this government coverage will be maintained. Any losses or damages incurred
by us could have a material adverse effect on our business. Any armed conflicts or political instability in the region would likely
negatively affect business conditions and could harm our results of operations.
in the past, the State of Israel and Israeli companies have been subjected to an economic boycott. Several countries still restrict
business with the State of Israel and with Israeli companies. These restrictive laws and policies may have an adverse impact on
our operating results, financial condition or the expansion of our business.
operations may be disrupted as a result of the obligation of Israeli citizens to perform military service.
Israeli citizens, including Or Eisenberg, our Acting Chief Executive Officer, Chief Financial Officer, Treasurer and Secretary,
are obligated to perform one month, and in some cases more, of annual military reserve duty until they reach the age of 45 (or
older, for reservists with certain occupations) and, in the event of a military conflict, may be called to active duty. In response
to increases in terrorist activity, there have been periods of significant call-ups of military reservists. It is possible that
there will be military reserve duty call-ups in the future. Our operations could be disrupted by such call-ups, which may include
the call-up of Or Eisenberg. Such disruption could materially adversely affect our business, financial condition and results of
a certain portion of our expenses is incurred in currencies other than the U.S. Dollar, our results of operations may be harmed
by currency fluctuations and inflation.
reporting and functional currency is the U.S. Dollar, but some portion of our clinical trials and operations expenses are in NIS
and Euro. As a result, we are exposed to some currency fluctuation risks, largely derived from our current and future engagements
for financing and distribution. Fluctuation in the exchange rates of foreign currency has an influence on the cost of goods sold
and our financing revenues and expenses. We may, in the future, decide to enter into currency hedging transactions to decrease
the risk of financial exposure from fluctuations in the exchange rate of the currencies mentioned above in relation to the U.S.
Dollar. These measures, however, may not adequately protect us from adverse effects.
may have difficulties enforcing a U.S. judgment, including judgments based upon the civil liability provisions of the U.S. federal
securities laws against us and our officers and directors or asserting U.S. securities laws claims in Israel.
directors and officers are not residents of the United States and our assets are located outside the United States. Service
of process upon our directors and officers and enforcement of judgments obtained in the United States against us, and our directors
and officers may be difficult to obtain within the United States. We have been informed by our legal counsel in Israel that
it may be difficult to assert claims under U.S. securities laws in original actions instituted in Israel or obtain a judgment
based on the civil liability provisions of U.S. federal securities laws. Israeli courts may refuse to hear a claim based
on a violation of U.S. securities laws against our officers and directors because Israel may not be the most appropriate forum
to bring such a claim. In addition, even if an Israeli court agrees to hear a claim, it may determine that Israeli law and
not U.S. law is applicable to the claim. If U.S. law is found to be applicable, the content of applicable U.S. law must
be proved as a fact, which can be a time-consuming and costly process. Certain matters of procedure will also be governed
by Israeli law. There is little binding case law in Israel addressing the matters described above. Israeli courts
might not enforce judgments rendered outside Israel, which may make it difficult to collect on judgments rendered against us and/or
our officers and directors.
among other reasons, including but not limited to, fraud, a lack of due process, a judgment which is at variance with another
judgment that was given in the same matter and if a suit in the same matter between the same parties was pending before a court
or tribunal in Israel, an Israeli court will not enforce a foreign judgment if it was given in a state whose laws do not provide
for the enforcement of judgments of Israeli courts (subject to exceptional cases) or if its enforcement is likely to prejudice
the sovereignty or security of the State of Israel.
1B. UNRESOLVED STAFF COMMENTS.
principal executive offices are located at 5b Hanagar Street, Hod Hasharon, Israel, 4527708 where we lease approximately 50 square
feet of office space for annual rent of approximately $30,000. Other than such office lease, we do not own or lease any material
tangible fixed assets. We believe that our existing facilities are suitable and adequate to meet our current business requirements.
In the event that we should require additional or alternative facilities, we believe that such facilities can be obtained on short
notice at competitive rates.
3. LEGAL PROCEEDINGS.
our knowledge, the ISA is conducting an administrative inquiry regarding Wize Israel’s public reports with the ISA in Israel
regarding its applicable regulatory path necessary for the marketing of LO2A for the treatment of DES in the United States.
As part of the inquiry, the ISA requested Wize Israel to provide certain documentation and has also questioned its officers with
respect to such reports. Wize Israel and its officers cooperated with the ISA and, at the ISA’s request, Wize Israel also
publicly filed a supplemental report to provide additional information in connection with the said regulatory path and marketing
plans, which we believe contained all the required information. As of the date of this Annual Report, it is uncertain whether
such inquiry will lead to any administrative enforcement proceedings by the ISA, if at all.
as described above, we are currently not, and have not been in the recent past, a party to any legal proceedings which may have
or have had in the recent past significant effects on our financial position or profitability. However, we have been in the past,
and may be from time to time in the future, named as a defendant in certain routine litigation incidental to our business.
4. MINE SAFETY DISCLOSURES.
5. MARKET FOR REGISTRANT’S COMMON EQUITY, RELATED STOCKHOLDER MATTERS AND ISSUER PURCHASES OF EQUITY SECURITIES.
Price for our Common Stock
Common Stock began trading on the OTC Pink under the symbol “OPLI” on January 25, 2012 through November 15, 2017,
and under the symbol “WIZP” from November 16, 2017 through January 3, 2018. Since January 4, 2018, our Common Stock
has been traded on the OTCQB under the symbol “WIZP.” Following the Reverse Stock Split, a “D” was placed
on our ticker symbol (WIZPD) for 20 business days from March 5, 2018, the effective date of the Reverse Stock Split. After 20
business days, the symbol will then change back to “WIZP.”
following table sets forth the range of the high and low closing prices of our Common Stock for the periods indicated, as adjusted
for the Reverse Stock Split.
Quarter (through March 28, 2018)
foregoing quotations were provided by Yahoo! Finance and the quotations reflect inter-dealer prices, without retail mark-up, mark-down
or commission and may not represent actual transactions. The last reported closing price per share of our Common Stock as quoted
on the OTCQB was $3.74 on March 28, 2018.
As of March 28, 2018, there were
approximately 72 stockholders of record holding 4,925,742 shares of our Common Stock. This number does not include an indeterminate
number of stockholders whose shares are held by brokers in street name. The holders of our Common Stock are entitled to one vote
for each share held of record on all matters submitted to a vote of stockholders. Holders of our Common Stock have no preemptive
rights and no right to convert their Common Stock into any other securities. There are no redemption or sinking fund provisions
applicable to our Common Stock.
have never paid any cash dividends on our Common Stock and do not anticipate paying any cash dividends on our Common Stock in
the foreseeable future. We intend to retain future earnings to fund ongoing operations and future capital requirements of our
business. Any future determination to pay cash dividends will be at the discretion of our Board and will be dependent upon our
financial condition, results of operations, capital requirements and such other factors as our Board deems relevant. Our ability
to pay cash dividends is subject to limitations imposed by state law. In addition, we are restricted from paying any dividends
without Rimon Gold’s consent so long as our loans from Rimon Gold have not been repaid in full.
Authorized for Issuance under Equity Compensation Plans
following table provides certain information with respect to all of the Company’s equity compensation plans in effect as
of December 31, 2017.
to be Issued
Warrants and Rights
Warrants and Rights
Reflected in Column (a)
|Equity compensation plans approved by security holders||
|| ||4,896|| ||
|| ||-|| |
|Equity compensation plans not approved by security holders||
|| || || ||
|| || || ||
|| || || |
|| ||4,896|| ||
|| ||-|| |
Sales of Equity Securities and Use of Proceeds
March 26, 2018, we issued 144,168 shares of Common Stock to an investor resulting from his exercise of PIPE Warrants for a total
exercise price of $0.3 million. This issuance was exempt under Section 4(a)(2) of the Securities Act of 1933, as amended.
6. SELECTED FINANCIAL DATA.
a “smaller reporting company,” the information required by this item is not required to be provided.
7. MANAGEMENT’S DISCUSSION AND ANALYSIS OF FINANCIAL CONDITION AND RESULTS OF OPERATIONS.
should read the following discussion and analysis of our financial condition and results of operations together with our audited
annual consolidated financial statements as of December 31, 2017 and December 31, 2016 and accompanying notes appearing elsewhere
in this Annual Report. This discussion and analysis contains forward-looking statements that involve risks, uncertainties and
assumptions. The actual results may differ materially from those anticipated in these forward-looking statements as a result of
certain factors, including, but not limited to, those set forth under “Risk Factors” and elsewhere in this Annual
Report. All amounts are in U.S. dollars and rounded.
are a clinical-stage biopharmaceutical company currently focused on the treatment of ophthalmic disorders, including DES. We have
in-licensed LO2A, a drug developed for the treatment of DES and other ophthalmological illnesses, including CCH and Sjögren’s.
have not generated any revenues from operations since its inception and although it anticipates generating some immaterial revenue
in Israel and the Ukraine during the first half of 2018, we do not currently expect to generate any significant revenues for the
foreseeable future, primarily because LO2A is still in early clinical stage development in the markets and for the indications
we are currently targeting. Our operating expenses have increased from $1,034,000 in the year ended December 31, 2016 to $1,481,000
in the year ended December 31, 2017. We will require significant additional capital and, assuming we will have sufficient liquidity
resources, we anticipate we will incur significantly higher costs in the foreseeable future, in order to finance our current strategic
plans, including the conduct of ongoing and future clinical trials as well as further research and development.
Wize Israel was deemed to be the
accounting acquirer in the Merger. The consolidated financial statements of Wize Israel included in this Annual Report are as
of and for the periods that are prior to the Merger, and have therefore, not been adjusted to reflect the impact of the Merger.
Ended December 31, 2017 Compared to Year Ended December 31, 2016
did not generate any revenues from operations during the years ended December 31, 2017 and 2016. We had no revenues primarily
because (1) from the time of the creditors’ arrangement in February 2015 until May 2015, when we (through Wize Israel) entered
into the LO2A License Agreement, Wize Israel did not conduct any business operations and (2) thereafter, currently, Wize Israel
is engaged primarily in research and development.
and development expenses. Research and development expenses were $450,000 for the year ended December 31, 2017, compared
to $240,000 for the year ended December 31, 2016, an increase of $210,000 or 87%. The increase in research and development expenses
is primarily related to the royalty expense of approximately $170,000 to Resdevco. For more information with respect to our expenses
in connection with entering into the LO2A License Agreement, please see Note 4 of the audited consolidated financial statements
of Wize Israel appearing elsewhere in this Annual Report.
and administrative expenses. General and administrative expenses were $1,031,000 for the year ended December 31, 2017,
compared to $794,000 for the year ended December 31, 2016, an increase of $237,000 or 30%. The increase in general and administrative
expenses during these periods is primarily related to increases in professional and legal services of $230,000.
Expenses, Net. Financial expenses, net were $1,485,000 for the year ended December 31, 2017 compared to financial expenses,
net of $105,000 for the year ended December 31, 2016, a change of $1,380,000 or 1314%. The increase in financial expenses during
this period is primarily related to increased amortization of the beneficial conversion feature (“BCF”) of $1,000,000,
change in the fair value of derivative liability for Investment Rights of $253,000 (this change resulted in financial income of
$76,000 during the year ended December 31, 2016) and loss from extinguishment of Convertible Loans of $61,000, which extinguishment
loss did not apply in 2016.
Loss. As a result of the foregoing, we incurred a net loss of $2,966,000 for the year ended December 31, 2017 compared to
a net loss of $1,139,000 for the year ended December 31, 2016, an increase in the net loss of $1,827,000 or 60%.
and Capital Resources
is the ability of a company to generate funds to support its current and future operations, satisfy its obligations, and otherwise
operate on an ongoing basis. Significant factors in the management of liquidity are funds generated by operations, levels of accounts
receivable and accounts payable and capital expenditures. Since the court-approved Creditors Arrangement completed in February
2015, as described below, we financed our operations primarily through equity and convertible debt financings in private placements,
as described below.
Capital and Cash Flows
of December 31, 2017 and December 31, 2016, we had $215,000 and $28,000 in cash and cash equivalents, respectively.
of December 31, 2017 and December 31, 2016, we had $3,204,000 and $406,000, respectively, of outstanding loans (including loans
from Wize Israel’s controlling shareholder as of December 31, 2016), including accrued interest and net of discounts, all
of which relates to the Convertible Loans, as described below.
of December 31, 2017 and December 31, 2016, we had ($3,103,000) and ($750,000) of working capital (deficit), respectively. As
of December 31, 2017, we had an accumulated deficit of $26,452,000. The increase in working capital deficit was primarily due
to additional loan amounts that have been received during the year ended December 31, 2017 from Ridge, and other lenders through
loans (including Convertible Loans) as described below, the implications of modifications of terms for such Convertible Loans,
reclassification of repurchase feature and Investment Rights and of license purchase obligations from being a non-current liability
to a current liability, based on the repayment terms under the LO2A License Agreement. Since the LO2A License Agreement relates
to an exclusive license to develop LO2A in the United States, Israel, Ukraine and China, and to purchase, market, sell and distribute
LO2A in finished product, which product has not yet been approved by the FDA, we determined, that the current status of LO2A is
in substance an In-Process Research and Development asset (“IPR&D”). As the IPR&D was received by Wize Israel
through a direct acquisition and not through a business combination and as it was determined that the IPR&D does not have
future alternative use, the acquisition cost, together with the related direct expenses (including the stock-based compensation)
were recorded as part of our R&D expenses during the year ended December 31, 2015.
following table presents the major components of net cash flows (used in) provided by operating, investing and financing activities
for the periods presented:
|| || ||
|| || |
|Net cash used in operating activities||
|Net cash used in investing activities||
|Net cash provided by financing activities||
Ended December 31, 2017 Compared to Year Ended December 31, 2016
the years ended December 31, 2017 and 2016, net cash used in operating activities was $1,357,000 and $874,000, respectively. The
increase in net cash used in operating activities was mainly due to an increase in net loss of $1,837,000 which was partly mitigated
by an increase in derivative liability and debt issuance costs related to Convertible Loans of $1,000,000, by an increase in change
in the fair value of derivative liability for Investment Rights of $329,000, and by an increase in fair value of license purchase
obligations of $146,000.
the years ended December 31, 2017 and 2016, net cash used in investing activities was $4,000 and $1,000, respectively.
the years ended December 31, 2017 and 2016, net cash provided by financing activities was $1,538,000 and $473,000, respectively.
Cash was provided in 2017 primarily by proceeds of $82,000 that were received from one of the Interim Loans and the net proceeds
of $625,000 that were received from the 2017 Loan Agreement. We (through Wize Israel) received $966,000 of proceeds in connection
with the 2017 PIPE, and $21,000 from the exercise of stock options into common stock. Cash was provided in 2016 primarily by net
proceeds from loans from Wize Israel’s controlling shareholder and from convertible loans. Repayment of the license purchase
obligation partly offset these net proceeds in both 2017 and 2016.
to management estimates, liquidity resources as of December 31, 2017 will not be sufficient to maintain our planned level of
operations for the next 12 months. In particular, we intend to seek the agreement of the lenders to convert the Convertible
Loans into shares before the maturity date and to raise additional funding. However, for a long-term solution, we will need
to seek additional capital for the purpose of implementing our business strategy and managing our business and developing
drugs. Conducting clinical trials and commercializing products is expensive and we will need to raise substantial additional
funds to achieve our strategic objectives. We have not yet generated any revenues from our current operations, and therefore
we are dependent upon external sources for financing our operations. We will require significant additional financing in the
near future. Additional financing may not be available on acceptable terms, if at all. Our future capital requirements as
well as the ability to obtain financing will depend on many factors, including those listed under Item 1A - “RISK
FACTORS – Risks Related to our Business,” beginning on page 36 of this Annual Report. As of December 31, 2017, we
had an accumulated deficit and a stockholders’ deficit. In addition, during the years ended December 31, 2017 and 2016,
we reported losses and negative cash flows from operating activities. Our management considered the significance of such
conditions in relation to our ability to meet our current and future obligations and determined that such conditions raise
substantial doubt about each our ability to continue as a going concern. As such, the reports of our independent registered
public accounting firms on the audited financial statements as of and for the year ended December 31, 2017 contain an
emphasis of matter paragraph regarding substantial doubt about our ability to continue as a going concern. Substantial doubt
about our ability to continue as a going concern could materially limit our ability to raise additional funds through
the issuance of new debt or equity securities or otherwise. Future reports on our financial statements may also include an
emphasis of matter paragraph with respect to our ability to continue as a going concern.
currently have no agreements, arrangements, or understandings with any person to obtain funds through bank loans, lines of credit,
or any other sources. Until we can generate significant continuing revenues, we expect to satisfy our future cash needs through
debt or equity financings, or by out-licensing its distribution rights. We cannot be certain that additional funding will be available
to us on acceptable terms, or at all. If funds are not available, we may be required to delay, reduce the scope of, or eliminate
one or more of our commercialization efforts.
are addressing our liquidity issues by implementing initiatives to raise additional funds as well as other measures that we believe
will allow us to continue as a going concern. Such initiatives may include monetizing of our assets, including the sale of the
Can-Fite shares that we currently own.
Financing Activities. The following is a summary of the equity and debt financings conducted by Wize Israel since the
December 2014, an Israeli court approved the Creditors’ Arrangement under the Israeli Companies Law between Wize Israel
(then known as Star Night Technologies Ltd.), its creditors and its shareholders, in which Wize Israel was purchased by a group
of investors led by Ridge. Upon the completion of the Creditors’ Arrangement, all of Wize Israel’s assets, rights
and obligations were transferred to the creditors’ arrangement fund, so that Wize Israel’s equity after the approval
of such arrangement was zero and Wize Israel remained a public shell company without any activity, rights or obligations. The
Creditors’ Arrangement was completed in February 2015. In connection with the Creditors’ Arrangement, on February
15, 2015, Wize Israel issued 692,307 ordinary shares of Wize Israel, in the aggregate, to Ridge, Zarachia, Avner Arazi (“Arazi”)
and Amir Bramli (“Bramli”, and together with Ridge, Zarachia and Arazi, the “2015 Investors”), in exchange
for their purchase of the public shell for NIS 1,800,000 (approximately $463,000). In addition, on April 7, 2015, for no consideration,
the 2015 Investors provided Wize Israel with a capital amount of NIS 4,056,000 (approximately $1,044,000) in cash.
of December 31, 2017, we (through Wize Israel) had a total principal and accrued interest balance of $1.415 million of loans outstanding
under the Convertible Loans described below, of which (1) Ridge extended a principal amount of NIS 1.0 million (approximately
$270,000), (2) Rimon Gold extended a principal amount of NIS 3.0 million (approximately $811,000), and (3) Fisher (not affiliated,
to Wize Israel’s knowledge, with Ridge or Rimon Gold) extended a principal amount of NIS 1.0 million (approximately $270,000).
Below is a summary of the material provisions of the Loan Agreements.
2016 Loan. On March 20, 2016, Wize Israel entered into a Convertible Loan (as amended on March 30, 2016) with Rimon Gold,
whereby Rimon Gold extended a loan in the principal amount of up to NIS 2 million (approximately $519,000), which bears interest
at an annual rate of 4% (the “2016 Loan”). Pursuant to the 2016 Loan Agreement, as modified by the 2017 Loan Agreement
and the 2017 Loan Amendment, both described below, the 2016 Loan has a maturity date of December 31, 2018.
the 2016 Loan Agreement, Rimon Gold had the right, at its sole discretion, to convert any outstanding portion of the 2016 Loan,
but not less than NIS 100,000 (approximately $26,000), into Wize Israel ordinary shares at a conversion price per share of NIS
15.2592 (approximately $3.84), subject to adjustments for stock splits and similar events set forth in the 2016 Loan Agreement.
As a result of the Merger and based on the Exchange Ratio, the conversion price per share for the 2016 Loan was adjusted to NIS
3.6 (approximately $0.96). As a result of the 2017 Loan Amendment, the aggregate principal amount of the 2016 Loan is $531,067
and the conversion price per share for the 2016 Loan was adjusted to $0.9768.
order to secure its obligations and performance pursuant to the 2016 Loan Agreement, Wize Israel recorded a first priority fixed
charge in favor of Rimon Gold on all of Wize Israel’s rights, including its distribution rights, under the LO2A License
Agreement, and a first priority floating charge on all of Wize Israel’s rights, title and interest in all of its assets,
as they may exist from time to time (the agreements relating to such charges being referred to as the “Security Agreements”).
Gold is entitled, under certain circumstances, to demand repayment of the 2016 Loan, including among others: (i) if Wize Israel
breaches or fails to perform or is shown to have made a false statement, under the 2016 Loan Agreement or the Security Agreements;
(ii) any failure of Wize Israel to make a timely payment; (iii) upon the appointment of a receiver; (iv) the imposition of a lien
on a material asset of Wize Israel; (v) if Wize Israel files a motion to stay proceedings; (vi) upon the expiration or termination
of the LO2A License Agreement or if any party is in material breach of the LO2A License Agreement or if any party notifies the
other of its intention to terminate the LO2A License Agreement; (vii) an adverse material change; and (viii) upon the non-performance
of Wize Israel pursuant to the 2017 Loan Agreement described below.
2016 Loan Agreement and the Security Agreements contain a number of other restrictive covenants that limit Wize Israel’s
operating flexibility. These covenants include, among other things, limitations on the creation of liens; on the incurrence of
indebtedness; on dispositions of assets, mergers, acquisitions and other change of control transactions; on changes in the general
nature of Wize Israel’s business; restrictions on payments to related parties; restrictions on conducting rights offerings,
and on the distribution of dividends.
addition, under the 2016 Loan Agreement, as modified by the 2017 Loan Agreement and the 2017 Loan Amendment, Rimon Gold has the
right, until June 30, 2019, to invest up to $796,601, in the aggregate, at an agreed price per share, which was adjusted based
on the Exchange Ratio from NIS 20.4 (approximately $6.00) to NIS 5.04 (approximately $1.44) and based on the 2017 Loan Amendment,
from NIS 5.04 to $1.308 (subject to adjustments in case of stock splits or similar events) (the “2016 Investment Right”).
See “-December 2017 Loan Amendment” below.
2017 Loan. On January 15, 2017, Wize Israel entered into the 2017 Loan Agreement with Ridge, and, by way of entering into
assignments and assumption agreements following such date, also with Rimon Gold and Fisher, whereby each of the lenders extended
a loan in the principal amount of up to NIS 1 million (approximately $283,000) and in the aggregate principal amount of up to
NIS 3 million (approximately $850,000), which bears interest at an annual rate of 4% (the “2017 Loan”, and together
with the 2016 Loan, the “Loans”)). Pursuant to the 2017 Loan Agreement and the 2017 Loan Amendment, the 2017 Loan
has a maturity date of December 31, 2018.
the 2017 Loan Agreement, each of the 2017 Lenders had the right, at its sole discretion, to convert any outstanding portion of
the 2017 Loan, but no less than NIS 100,000 (approximately $28,000), that the lender provided to Wize Israel (each such portion
converted, the into Wize Israel ordinary shares at a conversion price per share equal to the lower of (1) NIS 24 (approximately
$6.72) and (2) the lowest price per share of Wize Israel in any offering made by Wize Israel following the date of the 2017 Loan
Agreement and through the date of such requested conversion, subject to adjustments for stock splits and similar events set forth
in the 2017 Loan Agreement (the “2017 Loan Conversion Price”). As a result of the 2017 PIPE (described below), the
2017 Loan Conversion Price for Rimon Gold, Fisher and Ridge was adjusted to NIS 16.8 (approximately $4.80), and as a result of
the Merger, the 2017 Loan Conversion Price of NIS16.8 (approximately $4.8) was adjusted in accordance with the Exchange Ratio
to NIS 4.05 (approximately $1.15). As a result of the 2017 Loan Amendment, the aggregate principal amount of the 2017 Loan is
$822,144 and the 2017 Loan Conversion Price was adjusted to $1.1112. See “-December 2017 Loan Amendment” below.
addition, under the 2017 Loan Agreement, as modified by the 2017 Loan Amendment, the 2017 Lenders have the right, until June 30,
2019, to invest up to $1,233,216, in the aggregate, at an agreed price per share equal to 120% of the applicable 2017 Loan Conversion
Price, which was adjusted based on the 2017 Loan Amendment, to a fixed exercise price of $1.308 (subject to adjustments in case
of stock splits or similar events) (the “2017 Investment Right” and, together with the 2016 Investment Right, the
“Investment Rights”). See “-December 2017 Loan Amendment” below.
is entitled, under certain circumstances, to demand repayment of the 2017 Loan, including: (i) if Wize Israel breaches or fails
to perform or is shown to have made a false statement, under the 2017 Agreement or the Security Agreements; (ii) any failure of
Wize Israel to make a timely payment; (iii) upon the appointment of a receiver; (iv) the imposition of a lien on a material asset
of Wize Israel; (v) if Wize Israel files a motion to freeze proceedings; and (vi) an adverse material change.
2017 Loan contains a number of restrictive covenants that limit Wize Israel’s operating flexibility. These covenants include,
among other things, limitations on the creation of liens; on the incurrence of indebtedness; on dispositions of assets, mergers,
acquisitions and other change of control transactions; on changes in the general nature of Wize Israel’s business; restrictions
on payments to related parties; and on the distribution of dividends. Wize Israel has complied with the aforementioned covenants
through the date of this Annual Report.
should be noted that, prior to entering into the 2017 Loan Agreement, Ridge provided the following three loans to Wize Israel,
all of which bore interest at an annual rate equal to the interest rates of the Israeli government bonds: (1) NIS 250,000 was
extended in November 2016, (2) NIS 300,000 was extended in December 2016 and (3) NIS 200,000 was extended in February 2017 (together,
the “Ridge Interim Loans”). On March 30, 2017, after Ridge already provided NIS 250,000 under the 2017 Loan Agreement
out of the NIS 1 million committed by Ridge thereunder, Ridge exercised its right to have the Ridge Interim Loans being treated
as a portion of the remaining NIS 1 million.
addition, as part of the 2017 Loan Agreement, Wize Israel and the other lenders agreed that (1) the security interests made under
the Security Agreements will also serve to secure the loans made by Rimon Gold under the 2017 Loan Agreement, and (2) Rimon Gold
will have the right to be repaid the full 2016 Loan prior to any repayment of the 2017 Loan.
2017 Loan Amendment. On December 21, 2017, we entered into an amendment (the “2017 Loan Amendment”) to the 2016
Loan Agreement and the 2017 Loan Agreement. Pursuant to the 2017 Loan Amendment, (i) the maturity date of the Loans was extended
from December 31, 2017 to December 31, 2018; (ii) the exercise period of the 2016 Investment Right was amended so that it shall
expire on June 30, 2019; (iii) the exercise period of the 2017 Investment Right was amended so that it shall expire, without the
need to first convert the 2017 Loan, on June 30, 2019; and (iv) the below terms of the Loans were amended to be denominated in
U.S. dollars instead of NIS:
||2016 Loan|| ||
||2017 Loan|| |
|Aggregate Principal Amount||
|Conversion Price Per Wize US Share||
|Aggregate Maximum Investment Right||
|Exercise Price of Investment Right||
Principal loan amount of $274,048 for each of the three 2017 Lenders.
Maximum Investment Right of $411,072 for each of the three 2017 Lenders.
Gold and Ridge Consents to the Merger Agreement. In connection with the Merger Agreement, Wize Israel sought and obtained
the written consents of Rimon Gold and Ridge to the transactions contemplated by the Merger Agreement. The consent provided by
Rimon Gold provided that it is based upon, among other things, the following obligations: (1) following the closing of the Merger
Agreement, we will assist Rimon Gold with its filing requirements, if any, with the SEC with respect to beneficial ownership and
similar reports; and (2) at closing of the Merger Agreement, we will execute and deliver to Rimon Gold the Wize Guaranty, which
we executed and delivered to Rimon Gold.
the Wize Guaranty, we irrevocably guarantee Wize Israel’s obligations to Rimon Gold under the Convertible Loans. In addition,
the Wize Guaranty contains a number of restrictive covenants that limit our operating flexibility. These covenants include, among
other things, limitations on the creation of liens; on the incurrence of indebtedness; on dispositions of assets, mergers, acquisitions
and other change of control transactions; on changes in the general nature of our business; and on the distribution of dividends.
Wize Israel has complied with the aforementioned covenants through the date of this Annual Report.
2017 PIPE. On June 23, 2017,
Wize Israel entered into a Private Placement Agreement (the “2017 PIPE Agreements”) with each of Yosef Eliyahu Peretz
(“Peretz”), Yaakov Zarachia (“Zarachia”), Simcha Sadan (“Sadan”) and Jonathan Brian Rubini
(“Rubini”, and together with Peretz, Zarachia and Sadan, the “2017 PIPE Investors”). Pursuant to the 2017
PIPE Agreements, the 2017 PIPE Investors invested a total of up to NIS 3.49 million (approximately $1 million) in exchange for
a total of 207,739 ordinary shares of Wize Israel, at a price per share of NIS 16.8 (approximately $4.8), with Peretz investing
NIS 490,000 (approximately $139,000) in exchange for the private placement of 29,167 ordinary shares of Wize Israel (the “Peretz
Financing”) and each of Zarachia, Sadan and Rubini (the “Other Investors”) investing NIS 1 million (approximately
$282,000) in exchange for the private placement of 59,524 ordinary shares of Wize Israel each (together, the “Other Financing”),
and together with the Peretz Financing, the “2017 PIPE”). At the Effective Time, the 207,739 ordinary shares
of Wize Israel that were issued to the 2017 PIPE Investors as part of the 2017 PIPE were automatically cancelled and converted,
based on the Exchange Ratio, into an aggregate of 860,987 shares of our Common Stock.
to the closing of the Merger, Wize Israel also undertook to cause us to grant PIPE Warrants to each of the 2017 PIPE Investors,
with each PIPE Warrant being exercisable into one share of our Common Stock, with a term of three years from the date of grant.
According to the 2017 PIPE Agreements, the number of PIPE Warrants and the exercise price thereof will reflect, prior to giving
effect to an adjustment based on the exchange ratio, (i) 30,625 warrants to Peretz and (ii) 62,500 warrants to each of the Other
Investors, each warrant exercisable into one ordinary share of Wize Israel, at an exercise price of NIS 28.8 per share (approximately
$8.4). Based on the Exchange Ratio, Peretz was granted 126,928 PIPE Warrants and each of the Other Investors was granted 259,036
PIPE Warrants, each at an exercise price of $1.9728. Consistent with the foregoing, we executed and delivered the PIPE Warrants
to the 2017 PIPE Investors on November 16, 2017.
June 22, 2017, Ridge provided notice to Wize Israel that it has waived its right to adjust the 2017 Loan Conversion Price in connection
with the Peretz Investment. On July 4, 2017, Wize Israel completed the Peretz Investment. However, Ridge did not waive its right
to adjust the 2017 Loan Conversion Price in connection with the Other Investments. On July 31, 2017, at a general meeting of the
shareholders of Wize Israel, the Other Investments was approved and on August 7, 2017 Wize Israel completed the Other Investments.
of December 31, 2017 and December 31, 2016, we did not have any off-balance sheet arrangements, as such term is defined under
Item 303 of Regulation S-K, that have or are reasonably likely to have a current or future effect on our financial condition,
changes in financial condition, revenues or expenses, results of operations, liquidity, capital expenditures or capital resources
that is material to investors.
Issued Accounting Pronouncements
information with respect to recent accounting pronouncements, see Note 2w to our audited consolidated financial statements for
the year ended December 31, 2017 appearing elsewhere in this Annual Report.
and measurement of the Loans (including modifications accounting). The proceeds received upon issuance of the 2016 Loan together
with a freestanding derivative financial instrument (derivative liability for the 2016 Investment Right) were allocated to the
financial instruments issued, based on the residual value method. The detachable derivative financial instrument was recognized
based on its fair value and the remaining amount was allocated to the 2016 Loan component.
Israel considered the applicability of the “Derivatives and Hedging” guidance and determined that the embedded
conversion feature of the 2016 Loan should not be separated from the host instrument because it qualifies for equity classification.
Furthermore, Wize Israel applied the “Beneficial Conversion Features” (“BCF”) guidance to determine
whether the conversion feature is beneficial to the investor.|
BCF was calculated by allocating the proceeds received in financing transactions to the 2016 Loan and to any detachable freestanding
financial instrument (derivative liability for the 2016 Investment Right) included in the transaction, and by measuring the intrinsic
value of the conversion option based on the effective conversion price as a result of the allocated proceeds.
intrinsic value of the conversion option was recorded as a discount on the 2016 Loan with a corresponding amount credited directly
to equity as additional paid-in capital. After the initial recognition, the discount on the 2016 Loan was amortized as interest
expense over the contractual term of the 2016 Loan by using the effective interest method.
Israel considered the applicability of the “Derivatives and Hedging” guidance and determined that the embedded
conversion feature of the 2017 Loan should not be separated from the host instrument because the embedded conversion option,
if freestanding, does not meet the definition of a derivative, since its terms do not require or permit net settlement. Furthermore
Wize Israel applied the BCF guidance to determine whether the conversion feature is beneficial to the investor.|
amount of the BCF with respect to the 2017 Loan was calculated at the commitment date, as the difference between the conversion
price (i.e. the entire proceeds received for the 2017 Loan) and the aggregate fair value of the Common Stock and other securities
(which consist of the 2017 Investment Right) into which the 2017 Loan is convertible. As such difference was determined to be
greater than the amount of the entire proceeds received for the 2017 Loan, the amount of the discount assigned to the BCF was
limited to the amount of the entire proceeds.
7A. QUANTITATIVE AND QUALITATIVE DISCLOSURES ABOUT MARKET RISK.
a smaller reporting company, we have elected not to provide the disclosure required by this item.
8. FINANCIAL STATEMENTS AND SUPPLEMENTARY DATA.
information required by this item is included in Item 15 of Part IV of this Annual Report and is incorporated into this item by
9. CHANGES IN AND DISAGREEMENTS WITH ACCOUNTANTS ON ACCOUNTING AND FINANCIAL DISCLOSURE.
9A. CONTROLS AND PROCEDURES.
of Disclosure Controls and Procedures
management, with the participation of our Acting Chief Executive Officer and Chief Financial Officer, has evaluated the effectiveness
of our disclosure controls and procedures (as defined in Rules 13a- 15(e) and 15d- 15(e) under the Securities Exchange Act of
1934, as amended (Exchange Act)), as of the end of the period covered by this Annual Report. Based on such evaluation,
our Acting Chief Executive Officer and Chief Financial Officer have concluded that as of December 31, 2017, our disclosure
controls and procedures are designed at a reasonable assurance level and are effective to provide reasonable assurance that information
we are required to disclose in reports that we file or submit under the Exchange Act is recorded, processed, summarized, and reported
within the time periods specified in the rules and forms of the Securities and Exchange Commission, and that such information
is accumulated and communicated to our management, including our Acting Chief Executive Officer and Chief Financial Officer, as
appropriate, to allow timely decisions regarding required disclosure.
Report on Internal Control over Financial Reporting
management is responsible for establishing and maintaining adequate internal control over financial reporting to provide reasonable
assurance regarding the reliability of our financial reporting and the preparation of financial statements for external purposes
in accordance with generally accepted accounting principles. Internal control over financial reporting includes those
policies and procedures that (i) pertain to the maintenance of records that in reasonable detail accurately and fairly reflect
the transactions and dispositions of the assets of our company; (ii) provide reasonable assurance that transactions are recorded
as necessary to permit preparation of financial statements in accordance with generally accepted accounting principles, and that
receipts and expenditures of the company are being made only in accordance with authorizations of our management and directors;
and (iii) provide reasonable assurance regarding prevention or timely detection of unauthorized acquisition, use or disposition
of the company’s assets that could have a material effect on the financial statements.
of its inherent limitations, internal control over financial reporting may not prevent or detect misstatements. Also, projections
of any evaluation of effectiveness to future periods are subject to the risk that controls may become inadequate because of changes
in conditions, or that the degree of compliance with the policies or procedures may deteriorate.
assessed our internal control over financial reporting as of December 31, 2017, the end of our fiscal year. Management based
its assessment on criteria established in Internal Control—Integrated Framework (2013) issued by the Committee of
Sponsoring Organizations of the Treadway Commission (COSO). Management’s assessment included evaluation of such
elements as the design and operating effectiveness of key financial reporting controls, process documentation, accounting policies,
and our overall control environment.
on our assessment, management has concluded that our internal control over financial reporting was effective, as of the end of
the fiscal year, to provide reasonable assurance regarding the reliability of financial reporting and the preparation of financial
statements for external reporting purposes in accordance with generally accepted accounting principles.
of Independent Registered Public Accounting Firm
Annual Report does not include an attestation report of the Company’s independent registered public accounting firm
regarding internal control over financial reporting. Management’s report was not subject to attestation by the Company’s independent
registered public accounting firm pursuant to the rules of the SEC, applicable to emerging growth companies that permit the Company
to provide only management’s report in this Annual Report.
in Internal Control
were no changes in our internal control over financial reporting identified in management’s evaluation pursuant to Rules 13a-15(d)
or 15d-15(d) of the Exchange Act during the fourth quarter of 2017 that materially affected, or are reasonably likely to materially
affect, our internal control over financial reporting.
on Effectiveness of Controls and Procedures and Internal Control over Financial Reporting
designing and evaluating the disclosure controls and procedures and internal control over financial reporting, management recognizes
that any controls and procedures, no matter how well designed and operated, can provide only reasonable assurance of achieving
the desired control objectives. In addition, the design of disclosure controls and procedures and internal control over financial
reporting must reflect the fact that there are resource constraints and that management is required to apply judgment in evaluating
the benefits of possible controls and procedures relative to their costs.
9B. OTHER INFORMATION.
10. DIRECTORS, EXECUTIVE OFFICERS AND CORPORATE GOVERNANCE.
and Executive Officers
forth below is certain information with respect to the individuals who are our directors and executive officers.
of the Board|
Chief Executive Officer, Chief Financial Officer, Treasurer and Secretary|
following is a brief account of the education and business experience during at least the past five years of each director and
executive officer, indicating the principal occupation during that period, and the name and principal business of the organization
in which such occupation and employment were carried out.
Mayron. Ron Mayron has served on our board since the closing of the Merger on November 15, 2017. Mr. Mayron has also served
as the Chairman of the Board of Wize Israel since February 24, 2015. Mr. Mayron has extensive, long-term experience in the pharmaceutical
and medical equipment arena and has held various, significant senior management positions, both local and global, in Teva Pharmaceutical
Industries Ltd. (“Teva”), from 1993 to 2014. During his career at Teva, Mr. Mayron served in various vice president
positions, with his last role being the Vice President of Israel and Africa and serving as the chief executive officer of Teva
Israel, a wholly owned subsidiary of Teva. Mr. Mayron is a founder and the current CEO of RonMed Ltd. Mr. Mayron serves as a director
of BioLight Life Sciences Ltd. (TASE: BOLT) and Chairman of IceCure Medical Ltd. (TASE: ICCM) and on several boards of directors
of private companies. He holds a B.Sc. in Industrial Engineering & Management from Ben Gurion University and an MBA from Tel-Aviv
University. Ron Mayron’s qualifications to serve on our Board of Directors include his expertise in the pharmaceutical and
medical equipment arena.
Belkin, M.A., M.D. Michael Belkin has served on our board since July 1, 2013. Dr. Belkin is, and has been since 1980,
a Professor, and since 2010, a Professor Emeritus, of Ophthalmology at Tel Aviv University in Tel Aviv, Israel, and the Director
of the Ophthalmic Technologies Laboratory at the university’s Eye Research Institute at the Sheba Medical Center since 1997.
Since 2006, Dr. Belkin also serves as a Senior Consultant to the Eye Research Institute at the Singapore National Eye Institute.
He was awarded a master’s degree in natural sciences by Cambridge University, England, and received a doctorate in medicine
from the Hebrew University of Jerusalem. Dr. Belkin previously served as Director of Research, Development and Non-Conventional
Warfare Medicine in the Israel Defense Forces Medical Corps. He was also the first full-time Director of the Tel Aviv University
Eye Research Institute, Chairman of the Tel-Aviv University Department of Ophthalmology and the President of the Israel Society
of Eye and Vision Research, of which he was one of the founders. Dr. Belkin is an author of over 250 scientific publications and
20 patents. He is an internationally recognized eye researcher and has received various research awards. His laboratory is dedicated
to enabling the transfer of technologies from university-level research to clinical practice by providing expertise and facilities
for laboratory, preclinical and clinical studies. He is an entrepreneur and advisor of several ophthalmic companies in the fields
of lasers, optics, ophthalmic devices, pharmaceutics and biotechnology. One of his ideas, the ExPRESS miniature glaucoma shunt,
is currently used worldwide. Dr. Belkin is an active, long-standing, member of the Association for Research in Vision and Ophthalmology
(ARVO), the American Academy of Ophthalmology, the American Glaucoma Society and many others. He serves as chairman and member
of various international and local scientific and professional committees as well as scientific journals’ editorial boards.
Dr. Belkin’s qualifications to serve on our Board of Directors include his expertise in ophthalmic medical research, his
medical experience, and his experience as an advisor to several ophthalmic companies.
Keret. Yossi Keret has served on our board since the closing of the Merger on November 15, 2017. Mr. Keret has served as the
Chief Executive Officer, Managing Director and Director of Weebit-Nano Ltd. (ASX:WBT) from August 2015 to October 2017. From
October 1996 to October 2015, Mr. Keret served as the Chief Financial Officer of numerous public and private companies, including
Eric Cohen Books Ltd. & Burlington English Ltd., Daimler Financial Services Israel Ltd., Pluristem Life Systems Inc. (NASDAQ:PST),
M.L.L. Software and Computers Industries Ltd. (TASE:MLL), Internet-Zahav Group, Ltd. (NASDAQ:IGLD) and Top Image Systems Ltd.
(NASDAQ:TISA). Mr. Keret commenced his career at Kost Forer Gabbay & Kasierer, registered public accounting firm, a member
firm of Ernst & Young Global. Mr. Keret holds a B.A. from Haifa University in Economics and Accounting and is a Certified
Public Accountant in Israel. Mr. Keret’s qualifications to serve on our Board of Directors include his expertise in financial
matters and his serving as the Chief Financial Officer in numerous private and public companies.
Franck Amouyal. Dr. Franck Amouyal has served on our board since the closing of the Merger on November 15, 2017. Dr. Amouyal
practices as a medical and surgical ophthalmologist in Israel at Neve Tsedek Medical Center since October 2016 and Koupat Holim
Clalit and Meuhedet since November 2016. From February 2016 to June 2016 he practiced as an ophthalmologist at Sourasky
Medical Center, Ichilov. He conducted his residency and fellowship at the Nord Hospital and La Timone Hospital in Marseille,
France, at the Lariboisière Hospital, Paris, France and in the Jules Stein Eye Institute, UCLA, California, USA, as a research
assistant. Dr. Amouyal is the author of over 10 scientific publications and is a member of the French Society of Ophthalmology
(SFO) and the Association for Research in Vision and Ophthalmology (ARVO). He also lectures on ophthalmology to optometrists,
nurses and medical students. Dr. Amouyal holds a First Cycle and a Second Cycle of Medical Studies degree from the Medical
University of Purpan, Toulouse, France. Dr. Amouyal’s qualifications to serve on our Board of Directors include his
expertise in ophthalmic medical research and his medical experience.
Zarzewsky. Joseph Zarzewsky has served on our board since the closing of the Merger on November 15, 2017. Mr. Zarzewsky has
served as the Vice President of Business Development at the Mitrelli Group (“Mitrelli”) since June 2010. He
has served as the Chairman of “SMAD”, a joint venture between Mitrelli and the Harbin Government, China, since June
2011. Mr. Zarzewsky has also served as the Chairman of the Investment Committee of the Harbin Israel Fund since 2012. He
has also previously served as the Vice President of marketing at Clal Insurance Enterprises Holdings Ltd. (TASE: CLIS) and as
the Vice President of Marketing for the Israel Postal Authority. Mr. Zarzewsky has served as a director of Excellence Underwriter
House Ltd. since 2007. In 2008, he was appointed as the Honorary Economic Advisor of the Harbin Government, China. In addition,
in June 2012, he was honored as an Honorary Citizen of Harbin, China. Mr. Zarzewsky holds an MA in Commercial Law from both the
University of Tel Aviv and University of California, Berkeley. Mr. Zarzewsky’s qualifications to serve on our Board
of Directors include his expertise in financial matters.
Danenberg. Noam Danenberg has served as our Chief Operating Officer since the closing of the Merger on November 15, 2017.
Mr. Danenberg has served as a strategic advisor of Wize Israel since April 2015. Mr. Danenberg co-founded
Panmed Inc. (“Panmed”) in January 2014, a company in the field of repositioning drugs activities. Since 2000, Mr.
Danenberg has provided private investment consulting services to numerous private and public companies through his wholly owned company, N. Danenberg Holding (2000) Ltd.
From May 2014 to January 2015, Mr. Danenberg served as a director of Go.D.M. Investments Ltd. (TASE: GODM). From 2000 to 2012,
Mr. Danenberg served as an investment advisor at International Software Consulting Limited and from 2004 to 2008 he
served as the Chairman and CEO of Fitracks Inc. From 2006 to 2012, he also served as the Chairman of the Board of Hawk
Medical Technologies Ltd. Mr. Danenberg holds a B.B.A. in Computer Science from the European University in Antwerp,
Belgium and an M.B.A. from the Boston University Brussels Graduate Center.
Eisenberg. Or Eisenberg has served as our Acting Chief Executive Officer, Chief Financial Officer, Treasurer and Secretary
since the closing of the Merger on November 15, 2017. Mr. Eisenberg has served as the Chief Financial Officer and Acting Chief
Executive Officer of Wize Israel since March 2015. From October 2010 to December 2014, he served as the controller of the Katzir
Fund Group. From March 2013 to December 2014, he served as either an external controller or Chief Financial Officer of a number
of public companies whose shares are listed for trading on the TASE. From October 2007 to October 2010, Mr. Eisenberg was an accountant
at Kost Forer Gabbay & Kasierer, a registered public accounting firm, a member firm of Ernst & Young Global. Mr. Eisenberg
holds a B.A. from Haifa University in Economics and Accounting and is a Certified Public Accountant in Israel.
maintain a Scientific Advisory Board consisting of internationally recognized scientists who advise us on the scientific and technical
aspects of our business. The Scientific Advisory Board reviews and consults with respect to projects and occasionally assesses
the value of new technologies and developments. In addition, individual members of the Scientific Advisory Board meet with us
periodically to provide advice in their particular areas of expertise. The Scientific Advisory Board consists of the following
Joseph Tauber, MD. Dr. Tauber joined our Scientific Advisory Board in March 2018. He has been a principal investigator
in over 125 research studies of high-risk corneal transplantation, inflammation and allergic eye diseases, corneal infectious
diseases and numerous studies related to DES. Dr. Tauber has written five book chapters and over 60 articles in ophthalmology
medical journals. He has been awarded the Heed Ophthalmic Foundation Fellowship Award and the National Eye Institute Individual
NRSA Award. Dr. Tauber received his doctorate from Harvard Medical School, his training in internal medicine at Beth Israel Hospital
and in ophthalmology at Tufts-New England Medical Center. He has served as Clinical Professor of Ophthalmology at Kansas University
School of Medicine and University of Missouri-Kansas City School of Medicine. Dr. Tauber specializes in anterior segment surgery,
corneal transplantation, the treatment of corneal and external diseases and laser vision correction procedures. A board-certified
ophthalmologist, Dr. Tauber is the Founder of Tauber Eye Center in Kansas City, Missouri.
Professor Janos Nemeth, MD.
Dr. Nemeth joined the Wize Israel Scientific Advisory Board in October 2015 and has been a member of our Scientific Advisory
Board since the closing of the Merger on November 16, 2017. He has performed clinical trials with LO2A in the treatment of CCH
and Sjögren’s demonstrating efficacy in these indications. He has been a principal investigator or co-investigator
in 25 ophthalmology clinical trials, most of them in Phase III. Dr. Nemeth has written and/or edited 10 books, authored 37 book
chapters, and authored 351 scientific articles. He has received numerous awards including the Chibret Award, the Dr. Ferenc Papolczy
Foundation First Prize, both in Hungary, as well as the Imre-Blaskovics Prize and the Schulek Vilmos Prize of the Hungarian Ophthalmological
Society and the Gábor Brooser Prize of the Hungarian Ophthalmological and Diabetes Societies. Dr. Nemeth is an ophthalmologic
surgeon and Board Member of the Drug Discovery and Safety Center at Semmelweis University, Budapest, Hungary. Dr. Nemeth received
his doctorate of medicine from the University of Szeged, Hungary. He was a professor of ophthalmology at the University of Szeged,
Semmelweis University and at Pazmany Peter Catholic University in Hungary. Dr. Nemeth’s research fields of interest include
numerous ophthalmic indications, including Sjögren’s and tear film dynamics.
Gideon Stein, MD. Dr. Stein joined the Wize Israel Scientific Advisory Board in August 2015 and has been a member of
our Scientific Advisory Board since the closing of the Merger on November 16, 2017. He has more than 15 years of experience in
drug development, marketing and business development in the biotech industry in public and private companies. Dr. Stein is a graduate
of the Faculty of Medicine at Tel Aviv University, with a specialization in otolaryngology and head and neck surgery. He holds
an MBA and MHA from Tel Aviv University. Currently, Dr. Stein is the Executive Director of Innovative Venture at Bioline Rx, an Israeli based drug development company. Dr. Stein is also the co-founder of ProJoint Medical Technologies and Tree Healing,
where he currently serves as the CEO.
Franck Amouyal is the son-in-law of Philippe Halfon, who is a business partner of Noam Danenberg (in businesses unrelated to Wize).
Otherwise, there are no family relationships among our executive officers and directors.
have been no events under any bankruptcy act, no criminal proceedings and no judgments, injunctions, orders or decrees material
to the evaluation of the ability and integrity of any of our directors, executive officers, or control persons during the past
are elected to hold office until such director’s successor is elected and qualified or until such director’s earlier
resignation or removal. Annual meetings of the stockholders, for the election of directors to succeed those whose terms
expire, are to be held at such time each year as designated by our Board of Directors, which date shall be within 13 months of
the last annual meeting of stockholders. Officers are elected by the Board of Directors, which is required to consider that
subject at its first meeting after every annual meeting of stockholders. Each officer holds his office until his successor
is elected and qualified or until his earlier resignation or removal.
are not aware of any legal proceedings in which any of our directors, officers or affiliates, any owner of record or beneficially
of more than five percent of any class of our voting securities, or any associate of any such director, officer, or affiliate
of our company, or security holder is a party adverse to us or our subsidiaries or has a material interest adverse to us or our
have not adopted a code of ethics that applies to our officers, directors and employees.
securities are not listed on a national securities exchange or in an inter-dealer quotation system which has requirements that
directors be independent. However, we have adopted the independence standards of the NASDAQ Capital Market to determine the independence
of our directors and those directors serving on any committee. These standards provide that a person will be considered an independent
director if he or she is not an officer of the company and is, in the view of the company’s board of directors, free of
any relationship that would interfere with the exercise of independent judgment. The Board of Directors has determined that each
of Dr. Michael Belkin, Yossi Keret, Dr. Franck Amouyal and Joseph Zarzewsky are independent as defined under the rules promulgated
by the NASDAQ Capital Market. Other than Mr. Amouyal and Mr. Zarzewsky, none of the independent directors has any relationship
with us besides serving on our Board of Directors. Dr. Franck Amouyal is the son-in-law of Philippe Halfon, who is a business
partner of Noam Danenberg. On June 19, 2017, Wize Israel entered into a finder’s fee agreement with Harbin Israel (Trading)
Ltd., an affiliate of Mr. Zarzewsky, pursuant to which Mr. Zarzewsky will receive a 5% royalty on all of Wize Israel’s revenues
to the extent such revenues are earned from relationships initiated by Mr. Zarzewsky and agreed to by Wize Israel. The term of
the agreement is for 12 months unless earlier terminated. Either party may terminate upon twenty-one days’ notice. Mr. Zarzewsky
introduced us to the Chinese Distributor. See Item 1 - “BUSINESS — Marketing and Sales,” beginning on page
18 of this Annual Report. The Board of Directors considered these relationships and determined that they would not interfere
with Mr. Amouyal’s or Mr. Zarzewsky’s exercise of independent judgment in carrying out the responsibilities of a director.
have determined that each of the directors is qualified to serve as a director of the Company based on a review of the experience,
qualifications, attributes and skills of each director. In reaching this determination, we have considered a variety of criteria,
including, among other things: character and integrity; ability to review critically, evaluate, question and discuss information
provided, to exercise effective business judgment and to interact effectively with the other directors; and willingness and ability
to commit the time necessary to perform the duties of a director.
the year ended December 31, 2017, our Board of Directors held one meeting. All of our directors attended such meeting.
Committee and Audit Committee Financial Expert
members of our Audit Committee are Yossi Keret, Joseph Zarzewsky and Dr. Franck Amouyal. Our Board of Directors has determined
that Yossi Keret is an “audit committee financial expert” as set forth in Item 407(d)(5) of Regulation S-K and that
all members of the Audit Committee are “independent” as defined by the rules of the SEC and the NASDAQ Capital Market
rules and regulations. Our Board of Directors has not yet adopted a written charter.
members of our Compensation Committee are Yossi Keret, Dr. Michael Belkin and Joseph Zarzewsky. The Board of Directors has determined
that all of the members of the Compensation Committee are “independent” as defined by the rules of the SEC and the
NASDAQ Capital Market rules and regulations. Our Board of Directors has not yet adopted a written charter.
plan to organize a nominating and corporate governance committee during the first half of 2018. Because of our small size, our
Board of Directors carries out the duties of the nominating and corporate governance committee. In selecting nominees for directorships,
our Board of Directors considers a broad range of characteristics related to qualifications, background and diversity of nominees
based on our current business needs. Our Board of Directors has not adopted written guidelines regarding nominees for director.
There have been no material changes to the procedures by which security holders may recommend nominees to our Board of Directors.
Leadership Structure and Role in Risk Oversight
accordance with our Bylaws, our Board of Directors appoints our officers, including our Chief Executive Officer, Chief Financial
Officer, and such other officers as the Board of Directors may appoint from time to time. Mr. Ron Mayron currently serves
as our Chairman of the Board and Mr. Or Eisenberg currently serves as our Acting Chief Executive Officer, Chief Financial Officer,
Treasurer and Secretary. Our Board of Directors periodically considers whether changes to our overall leadership structure are
Chairman is responsible for chairing meetings of the Board of Directors. Our Bylaws provide that if our Chairman is unable
to preside at meetings of the Board of Directors, our Chief Executive Officer, if such officer is a director, shall preside at
such meetings. Our Chairman is also responsible for chairing meetings of stockholders. In his absence, the Board of
Directors may appoint another party to chair the stockholders’ meeting.
is inherent with every business, and how well a business manages risk can ultimately determine its success. We face a number
of risks, including strategic risks, enterprise risks, financial risks, regulatory risks, and others. Management is responsible
for the day-to-day management of risks the company faces, while our Board of Directors, as a whole, has responsibility for the
oversight of risk management. In its risk oversight role, our Board of Directors has the responsibility to satisfy itself
that the risk management processes designed and implemented by management are adequate and functioning as designed.
Board of Directors believes that full and open communication between management and the Board of Directors is essential for effective
risk management and oversight. Senior management attends Board of Directors meetings and is available to address any questions
or concerns raised by our Board of Directors on risk management-related and any other matters.
by Stockholders with Directors
encourage stockholder communications to our Board of Directors and/or individual directors. Stockholders who wish to communicate
with our Board of Directors or an individual director should send their communications to the care of Secretary, Wize Pharma,
Inc., 5b Hanagar Street, Hod Hasharon, Israel 4527708. The Secretary will maintain a log of such communications and will
transmit as soon as practicable such communications to the Chairman of the Board or to the identified individual director(s),
although communications that are abusive, in bad taste or that present safety or security concerns may be handled differently,
as determined by the Secretary.
Attendance at Annual Meetings
will make every effort to schedule our annual meeting of stockholders at a time and date to accommodate attendance by directors
taking into account the directors’ schedules. While all directors are encouraged to attend our annual meeting of stockholders,
there is no formal policy as to their attendance at annual meetings of stockholders.
Beneficial Ownership Reporting Compliance
16(a) of the Exchange Act requires our directors, executive officers and persons who own more than 10% of our Common Stock to
file with the SEC reports of ownership and changes in ownership of our Common Stock. Our directors, executive officers and greater
than 10% beneficial owners of our Common Stock are required by SEC regulation to furnish us with copies of all Section 16(a)
reports they file. Based solely upon information furnished to us and contained in reports filed with the SEC, we believe that
all Section 16(a) reports of our directors, executive officers and greater than 10% beneficial owners were filed timely for
the fiscal year ended December 31, 2017.
11. EXECUTIVE COMPENSATION.
following table sets forth information concerning the annual compensation awarded to, earned by, or paid to the following named
executive officers for all services rendered in all capacities to us for the years ended December 31, 2017 and 2016. The amounts
set forth for Mr. Eisenberg and Mr. Danenberg were originally denominated in NIS and were translated into U.S. Dollars at the
average current exchange rate for each year.
Other Compensation ($)
Acting Chief Executive Officer and Chief
Danenberg, Chief Operating Officer and Strategic
Chairman and Chief Executive
Weinstein Former Chief Financial
shown represent consulting fees earned or paid during the fiscal year.|
the aggregate grant date fair value of option awards granted during the relevant fiscal year calculated in accordance with
FASB ASC Topic 718.|
represents car allowance.|
Eisenberg was appointed as our Acting Chief Executive Officer and Chief Financial Officer on November 16, 2017 in connection
with the Merger. He has served as the Acting Chief Executive Officer and Chief Financial Officer of Wize Israel since 2015.|
services of Mr. Danenberg are provided via N. Danenberg Holdings (2000) Ltd. (“Danenberg Holdings”), a services
company wholly owned by Mr. Danenberg, pursuant to the terms of the services agreement by and between Wize Israel and Danenberg
Holdings. Pursuant to such agreement, Mr. Danenberg shall dedicate 80% of his time to us. Mr. Danenberg was appointed
as our Chief Operating Officer on November 16, 2017 in connection with the Merger. He has served as a strategic advisor to
Wize Israel since 2015.|
Fishman served as our Chief Executive Officer until her resignation on November 16, 2017 in connection with the Merger. As
Chief Executive Officer of Can-Fite, our former majority stockholder and parent, Dr. Fishman was compensated by Can-Fite,
for her services to us as Chairman of the Board and Chief Executive Officer.|
Weinstein served as our Chief Financial Officer until his resignation on November 16, 2017 in connection with the Merger.
Mr. Weinstein is also the controller of Can-Fite, our former majority stockholder and parent, and was compensated by
Can-Fite for services provided to Can-Fite.|
as set forth below, we have not entered into any employment agreements with the named executive officers listed in the table above.
Agreement of Or Eisenberg
Eisenberg has served as Wize Israel’s Chief Financial Officer and Acting Chief Executive Officer since March 2015 and as
our Financial Officer and Acting Chief Executive Officer since the Merger. Mr. Eisenberg’s employment agreement is with
Wize Israel. The term of Mr. Eisenberg’s employment is for three years commencing from April 1, 2015. Either party may terminate
the agreement upon 90 days prior notice. Wize Israel may terminate the agreement immediately, if Mr. Eisenberg: (i) committed
a criminal offense relating to his relationship with Wize Israel or of moral turpitude, (ii) breached his duty of loyalty or his
confidentiality, non-competition, non-solicitation or maintenance of Wize Israel’s reputation undertakings to Wize Israel,
(iii) caused harm to Wize Israel, its funds, property, assets, employees or customers, or (iv) took action that would cause him
to lose his right to severance pay under Israeli law.
Eisenberg is entitled to a fixed monthly salary of NIS 30,000 (approximately $8,500) and an additional monthly amount of NIS 10,000
(approximately $2,900), for so long as Mr. Eisenberg continues to serve as the Acting Chief Executive Officer of Wize Israel.
The monthly bonus does not entitle Mr. Eisenberg to any Wize Israel contribution or pension rights. Mr. Eisenberg may be entitled
to a 10% increase of his monthly salary upon Wize Israel completing a Phase II clinical trial for the treatment of CCH. Other
targets described in Mr. Eisenberg’s employment agreement are no longer achievable. As part of the terms of Mr. Eisenberg’s
employment, Mr. Eisenberg is entitled to certain benefits, including but not limited to vacation days, sick days, an education
fund, a pension fund, severance pay, convalescence pay, certain business expense reimbursements, vehicle expenses up to a sum
of NIS 3,000 (approximately $900) per month, internet, a mobile phone, various insurance policies including disability insurance,
indemnification, and business related travel expenses up to $10,000 on an annual basis.
addition, Mr. Eisenberg is entitled to a bonus of up to 0.25% of the consideration paid in connection with a material transaction
of Wize Israel or a Wize Israel subsidiary, including the sale of a subsidiary, sale of operations, asset sale related to the
field of operation, sale of shares, a merger of Wize Israel, Wize Israel entering into a material license agreement, raising capital
and/or the financing of Wize Israel (the “Annual Eisenberg Grant”). In the event of an offering of a subsidiary of
Wize Israel, Mr. Eisenberg is entitled to a grant of up to 0.25% of the post offering holdings of Wize Israel in such subsidiary
in the event the process of such offering commenced during the term of Mr. Eisenberg’ service to Wize Israel (the “Subsidiary
Eisenberg Grant”). The maximum Annual Eisenberg Grant together with the Subsidiary Eisenberg Grant may not exceed in any
fiscal year NIS 8 million (approximately $2.3 million), to all of the officers of Wize Israel, in the aggregate. Neither the Annual
Eisenberg Grant nor the Subsidiary Eisenberg Grant was payable in connection with the closing of the Merger. In addition, Mr.
Eisenberg was entitled to an option to purchase 9,583 ordinary shares of Wize Israel, which was granted to Mr. Eisenberg in September
2015. In connection with the Merger and for no consideration, on June 19, 2017, Mr. Eisenberg agreed, subject to and effective
upon the closing of the Merger, to cancel any and all options or other rights to purchase Wize’s shares that are not exercised
at least seven business days prior to the closing of the Merger. Mr. Eisenberg did not exercise his options prior to the closing
of the Merger.
Agreement of Noam Danenberg
Israel entered into a services agreement with Danenberg Holdings, a services company wholly owned by Mr. Noam Danenberg with respect
to the engagement of Mr. Danenberg to provide services to Wize Israel, which include strategic consulting, business development
in Israel and abroad, and raising funds for Wize Israel. The agreement was entered into on April 29, 2015. Mr. Danenberg is required
to devote at least 80% of his time to providing services to Wize Israel. Mr. Danenberg has served as Wize Israel’s strategic
advisor since April 2015. The term of Mr. Danenberg’s services is for three years commencing on April 29, 2015. Either party
may terminate the agreement upon 90 days prior notice. Wize Israel may terminate the agreement immediately, if Mr. Danenberg or
Danenberg Holdings: (i) committed a criminal offense relating to his or its, as applicable, relationship with Wize Israel, (ii)
breached his or its, as applicable, duty of trust to Wize Israel, or (iii) caused harm to Wize Israel, its funds, property, assets,
employees or customers. In addition, Wize Israel may terminate the agreement immediately, if: (i) a liquidator or receiver was
appointed for Danenberg Holdings, (ii) Mr. Danenberg ceases to control Danenberg Holdings, or (iii) Mr. Danenberg took action
that would cause him to lose his right to severance pay under Israeli law, if he was an employee of Wize Israel.
Holdings is entitled to a fixed monthly consulting fee of NIS 25,000 (approximately $7,150). Danenberg Holdings may be entitled
to a 10% increase in consulting fees upon each of (i) raising capital and/or financing for Wize Israel in an amount of at least
NIS 6 million (approximately $1.8 million), which condition was met in August 2017, and (ii) Wize Israel completing a Phase II
clinical trial for the treatment of CCH. Other targets described in Danenberg Holdings’ services agreement are no longer
achievable. Danenberg Holdings is also entitled to certain benefits, including but not limited to certain business expense reimbursements
up to a sum of NIS 3,000 (approximately $900) per month, vehicle expenses up to a sum of NIS 3,000 (approximately $900) per month,
internet, a mobile phone, professional training, and business related travel expenses up to $10,000 on an annual basis. In addition,
Danenberg Holdings is entitled to a bonus of up to 0.5% of the consideration paid in connection with a material transaction of
Wize Israel or a Wize Israel subsidiary, including the sale of a subsidiary, sale of operations, asset sale related to the field
of operation, sale of shares, a merger of Wize Israel, Wize Israel entering into a material license agreement, raising capital
and/or the financing of Wize Israel (the “Annual Danenberg Grant”). In the event of an offering of a subsidiary of
Wize Israel, Danenberg Holdings is entitled to a grant of up to 0.5% of the post offering holdings of Wize Israel in such subsidiary
in the event the process of such offering commenced during the term of Mr. Danenberg’s services to Wize Israel (the “Subsidiary
Danenberg Grant”). The maximum Annual Danenberg Grant together with the Subsidiary Danenberg Grant may not exceed in any
fiscal year NIS 8 million, (approximately $2.3 million) to all of the officers of Wize Israel, in the aggregate. Neither the Annual
Danenberg Grant nor the Subsidiary Danenberg Grant was payable in connection with the closing of the Merger.
of the above agreements incorporates the terms and provisions of a customary employee proprietary information, invention, non-competition
and non-solicitation between Wize Israel and the executive.
Equity Awards at Fiscal Year-End
following table provides information regarding all outstanding equity awards for our named executive officers as of December 31,
options were granted on July 1, 2013 and vested as follows: 1/12th vested on September 30, 2013 and 1/12th of the
total options vested on the last day of each of the eleven quarters thereafter.|
options were granted on May 9, 2013 with 50% vested upon grant and the remaining 50% vesting on a quarterly basis over a three
following table provides information regarding the total compensation that we paid or awarded to our non-executive directors during
the year ended December 31, 2017.
Michael Belkin (3), (4)
Franck Amouyal (6)
the aggregate grant date fair value of option awards granted during the relevant fiscal year calculated in accordance with
FASB ASC Topic 718.|
Cohn and Partners, an Israeli partnership, of which Ilan Cohn, Ph.D. is a partner provides intellectual property legal services
to us in the ordinary course of business.|
connection with the appointments of Drs. Kornberg and Belkin, we entered into agreements to pay director fees for attendance
at board meetings or any committee of the board. Drs. Kornberg and Belkin will each receive $2,000 for attendance in person
at a meeting of the Board of Directors, $750 for attendance by telephone at a meeting of the Board of Directors, and $750
for attendance at each meeting of any committee of the Board of Directors. Dr. Kornberg resigned from the Board of Directors
on November 16, 2017 and the agreement with Dr. Belkin was terminated on February 22, 2018.|
July 1, 2013, we granted to Dr. Belkin options to purchase 2,176 shares of our Common Stock at $159.12 per share. The options
are fully vested and will be expire on the ten year anniversary of the grant date.|
Mayron received NIS 32,866 (approximately $9,400) in cash from Wize Israel for serving as the Chairman of the Board of Wize
Israel. Mr. Mayron has served on the Board of Directors of Wize Israel since February 24, 2015. |
of Ron Mayron, Yossi Keret, Dr. Franck Amouyal and Joseph Zarzewsky has served on our
Board of Directors since November 16, 2017 and received $750 from us in 2017. |
Agreement with Ron Mayron
Israel entered into a services agreement with Ron Med Ltd. (“RML”), a services company wholly owned by Mr. Mayron,
with respect to the engagement of the services of Mr. Mayron which include active chairman of the board of directors services
to Wize Israel and to all subsidiaries and/or related companies of Wize Israel to the extent required from time to time by Wize
Israel and in accordance with its needs. Mr. Mayron is required to devote at least 20% of his time to providing services
to Wize Israel. Mr. Mayron has served as Wize Israel’s Chairman of the Board since February 24, 2015. The term
of Mr. Mayron’s services is for three years commencing on March 31, 2015. Either party may terminate the agreement
upon 90 days prior notice. Wize Israel may terminate the agreement immediately, if Mr. Mayron or RML: (i) committed a criminal
offense relating to his or its, as applicable, relationship with Wize Israel, (ii) breached his or its, as applicable, duty of
trust to Wize Israel, or (iii) caused harm to Wize Israel, its funds, property, assets, employees or customers. In addition, Wize
Israel may terminate the agreement immediately, if: (i) a liquidator or receiver was appointed for RML, (ii) Mr. Mayron ceases
to control RML, (iii) Mr. Mayron took action that would cause him to lose his right to severance pay under Israeli law, if he
was an employee of Wize Israel, or (iv) Mr. Mayron ceased to be qualified to be Wize Israel’s Chairman of the Board.
Mayron was initially entitled to a fixed monthly payment of NIS 20,000 (approximately $5,700) (the “Mayron Monthly Payment”)
for his services to Wize Israel, In November 2016, the shareholders of Wize Israel approved the revised compensation terms of
Mr. Mayron, which included that effective as of January 1, 2016, Mr. Mayron would no longer receive the Mayron Monthly Payment,
but would rather receive a payment in accordance with the Compensation Regulations promulgated under the Israeli Companies Law,
consisting of an annual fee of approximately NIS 20,000 (approximately $5,700) and a per meeting fee of approximately NIS 1,100
(approximately $300), which payment was no longer payable to him as of the Closing Date. In addition, Mr. Mayron was granted an
option to purchase 300,000 ordinary shares of Wize Israel.
addition, Mr. Mayron is entitled to a bonus of up to 0.25% of the consideration paid in connection with a material transaction
of Wize Israel or a Wize Israel subsidiary, including the sale of a subsidiary, sale of operations, asset sale related to the
field of operation, sale of shares, a merger of Wize Israel, Wize Israel entering into a material license agreement, raising capital
and/or the financing of Wize Israel (the “Annual Mayron Grant”). The Annual Mayron Grant was not payable in connection
with the Merger. In addition, Mr. Mayron is entitled to an option to purchase 105,000 ordinary shares of Wize Israel (the “Capital
Remuneration”), which was granted to Mr. Mayron in September 2015. In connection with the Merger and for no consideration,
on June 19, 2017, Mr. Mayron agreed, subject to and effective upon the closing of the Merger, to cancel any and all options or
other rights to purchase Wize Israel’s shares that are not exercised at least seven business days prior to the closing of
the Merger. On October 25, 2017 and on November 8, 2017, Mr. Mayron exercised options to purchase a total of 182,056 ordinary
shares of Wize Israel, some of which he sold prior to the Closing Date. The remaining shares of Wize Israel that Mr. Mayron held
as of the Closing Date were converted into shares of our Common Stock upon the closing of the Merger. The maximum Annual Mayron
Grant together with the Capital Remuneration may not exceed in any fiscal year NIS 8 million (approximately $2.3 million), to
all of the officers of Wize Israel, in the aggregate.
Mayron’s agreement incorporates the terms and provisions of a customary employee proprietary information, invention, non-competition
and non-solicitation between Wize Israel and its executives.
Fee Agreement with Joseph Zarzewsky
June 19, 2017, Wize Israel entered into a finder’s fee agreement with Harbin Israel (Trading) Ltd., an affiliate of Mr.
Zarzewsky, pursuant to which Mr. Zarzewsky will receive a 5% royalty on all of Wize Israel’s revenues to the extent such
revenues are earned from relationships initiated by Mr. Zarzewsky and agreed to by Wize Israel. The term of the agreement is for
12 months unless earlier terminated. Either party may terminate upon twenty-one days’ notice. Mr. Zarzewsky introduced us
to the Chinese Distributor. See “BUSINESS — Marketing and Sales,” beginning on page 18 of this prospectus.
February 22, 2018, our compensation committee determined to pay each director an annual fee of $10,000 in cash in addition to
receiving $800 in cash per in person meeting, $400 per signed unanimous consent and $600 per telephonic meeting, with respect
to meetings and/or signed resolutions, as applicable, of the Board of Directors or a committee of the Board of Directors.
have also purchased Directors and Officers insurance to cover the potential liability of our directors and executive officers.
Prior to the Effective Time of the Merger, Wize Israel purchased, for a period of seven years following the Effective Time, a
directors’ and officers’ liability “tail” insurance policy or policies covering the then current and former
directors or officers of Wize Israel for events occurring at or prior to the Effective Time, which insurance will be of at least
the same coverage and amounts and contain terms and conditions which are no less advantageous to such persons than the coverage,
amounts, terms and conditions of the directors’ and officers’ liability insurance policy maintained by Wize Israel
as of the date of the Merger Agreement.
12. SECURITY OWNERSHIP OF CERTAIN BENEFICIAL OWNERS AND MANAGEMENT AND RELATED STOCKHOLDER MATTERS.
following table sets forth information as of March 28, 2018 regarding the beneficial ownership of our Common Stock by (i)
those persons who are known to us to be the beneficial owner(s) of more than 5% of our Common Stock, (ii) each of our
directors and named executive officers, and (iii) all of our directors and executive officers as a group. Except as otherwise
indicated, the beneficial owners listed in the table below possess the sole voting and dispositive power in regard to such
shares and have an address of c/o Wize Pharma, Inc., 5b Hanagar Street, Hod Hasharon, Israel 4527708. As of March 28, 2018,
there were 4,925,742 shares of our Common Stock outstanding.
ownership is determined in accordance with the rules of the SEC and generally includes voting or investment power with respect
to securities. Shares of our Common Stock subject to options, warrants, notes or other conversion privileges currently exercisable
or convertible, or exercisable within 60 days of the date of this table, are deemed outstanding for computing the percentage of
the person holding such option, warrant, note, or other convertible instrument but are not deemed outstanding for computing the
percentage of any other person. Where more than one person has a beneficial ownership interest in the same shares, the sharing
of beneficial ownership of these shares is designated in the footnotes to this table. Unless otherwise indicated in the
footnotes to this table, we believe that each of the stockholders named in this table has sole voting and investment power with
respect to the shares indicated as beneficially owned.
|Name and Address of Beneficial Owner
||Amount and Nature of Beneficial Ownership
||Percent of Class
|5% and Greater Shareholders
|Rimon Gold Assets Ltd. (1)
|Ridge Valley Corporation (2)
|Yaakov Zarachia (3)
|Simcha Sadan (4)
|Shimshon Fisher (5)
|Jonathan Rubini (6)
|Erez Haver, Adv. in trust for Amir Bramli (7)
|Can-Fite BioPharma Ltd. (8)
|Erez Haver, Adv. and Yehuda Brami, Adv., in trust for Avner Arazi (9)
|Named Executive Officers and Directors
|Dr. Franck Amouyal
|Dr. Michael Belkin (10)
|Noam Danenberg (11)
|Executive Officers and Directors as a Group (7 Persons)
ownership of less than 1%|
(i) 217,442 shares of Common Stock, (ii) 848,251 shares of Common Stock issuable upon the conversion of the Convertible Loans
and (iii) 700,431 shares of Common Stock issuable upon the exercise of the Investment Rights. Rimon Gold is an Israeli private
company wholly owned by the Goldfinger Trust (the “Trust”), whose trustee is Abir Raveh (the “Trustee”)
and whose beneficiary is Yair Goldfinger. The Trust directs the management of Rimon Gold, its investment and voting
decisions and the Trustee directs the management of the Trust, its investment and voting decisions. The address
of Rimon Gold, the Trust and the Trustee is 32 Habarzel, Tel Aviv, Israel. Mr. Goldfinger does not direct the management of
Rimon Gold, the Trust or the Trustee, its investment or voting decisions and disclaims beneficial ownership of the shares
reported in this table. |
(i) 1,044,509 shares of Common Stock, (ii) 258,137 shares of Common Stock issuable upon the conversion of the Convertible
Loans and (iii) 91,103 shares of Common Stock issuable upon the exercise of the Investment Rights. Ridge is a Seychelles corporation,
whose address is Room 206, Premier Building, P.O Box 332, Victoria, Mahe, Seychelles. Priscilla Julie is the sole director
of Ridge and holds the voting and dispositive power of the shares of Common Stock beneficially owned by Ridge. Noam Danenberg,
our Chief Operating Officer, is also the son-in-law of Mrs. Hanna Harpaz, who owns 49% of Ridge.|
(i) 515,496 shares of Common Stock and (ii) 259,036 shares of Common Stock issuable upon
the exercise of the PIPE Warrants. The address for Mr. Zarachia is 10 Tzemach
Tzedek Street, Lod, Israel.
||Represents (i) 567,975 shares of Common Stock and (ii) 114,868 shares of Common Stock issuable upon the
exercise of the PIPE Warrants. The address for Mr. Sadan is Hashunit 10, Herzliya, Israel.|
(i) 258,115 shares of Common Stock issuable upon the conversion of the Convertible Loans and (ii) 308,377 shares of Common
Stock issuable upon the exercise of the Investment Rights. The address of Mr. Fisher is 3 HaRav Shmuel Rozovski
Street, Bnei Brak, Israel.|
(i) 246,702 shares of Common Stock and (ii) 259,036 shares of Common Stock issuable upon the exercise of the PIPE Warrants.
The address for Mr. Rubini is 2655 Marston Drive, Anchorage, Alaska 99517.|
our knowledge, the shares of Common Stock are held by Erez Haver, Adv., who was court-appointed as liquidator of a company
affiliated with, and holds such shares in trust for, Amir Bramli. The address of Advocate Erez Haver is APM House, 18 Raoul
Wallenberg St., Building D, 6th floor, Tel Aviv, Israel.|
address of Can-Fite BioPharma Ltd. is 10 Bareket Street, Kiryat Matalon, P.O. Box 7537, Petah-Tikva, 49170, Israel.|
our knowledge, the shares of Common Stock are held by Erez Haver, Adv. and Yehuda Bramli,
Adv., who were court-appointed as joint receivers on the assets of, and hold such shares
in trust for, Avner Arazi. The address of Advocate Erez Haver is APM House, 18 Raoul
Wallenberg St., Building D, 6th floor, Tel Aviv, Israel.
2,176 shares of Common Stock issuable upon exercise of vested options.|
shares of Common Stock are held by Mr. Danenberg through a company where Mr. Danenberg holds a minority interest and he does
not serve as a director or an officer. See footnote 2 above.|
Compensation Plan Information
Stock Incentive Plan
February 6, 2012, our Board of Directors and stockholders adopted the 2012 Stock Incentive Plan (the “2012 Plan”).
The purpose of the 2102 Plan is to advance the interests of our stockholders by enhancing the Company’s ability to attract,
retain and motivate persons who are expected to make important contributions to us and by providing such persons with equity ownership
opportunities and performance-based incentives that are intended to better align the interests of such persons with those of our
stock option granted shall be exercisable at such times and terms and conditions as the Board of Directors may specify in the
applicable option agreement, provided that no option will be granted with a term in excess of 10 years. Upon the adoption of the
2012 Plan, we reserved for issuance 45,370 shares of Common Stock. There are 45,370 shares of Common Stock authorized for non-statutory
and incentive stock options, restricted stock units, and stock grants under the 2012 Plan, which are subject to adjustment in
the event of stock splits, stock dividends, and other situations. As of December 31, 2017, we had 40,474 shares of Common Stock
available for future grant under the 2012 Plan. During the years ended December 31, 2017 and 2016, we did not grant any new stock
2012 Plan is administered by our Board of Directors. The persons eligible to participate in the 2012 Plan are as follows: all
of our employees, officers and directors, as well as consultants and advisors to the Company (as such terms consultants and advisors
are defined and interpreted for purposes of Form S-8 under the Securities Act of 1933, as amended, or any successor form) are
eligible to be granted Awards under the 2012 Plan. Each person who is granted an Award under the 2012 Plan is deemed a “Participant.”
“Award” means Options (as defined in Section 5(a)), “Restricted Stock” (as defined in Section 6(a)), “Restricted
Stock Units” (as defined in Section 6(a)), “Other Stock-Based Awards” (as defined in Section 7(a)) and “Performance
Awards” (as defined in Section 8(a)). follows: (a) our employees and any of our subsidiaries; (b) non-employee members of
the board or non-employee members of our Board of Directors or any of our subsidiaries; and (c) consultants and other independent
advisors who provide services to us or any of our subsidiaries.
2012 Plan will continue in effect until all of the stock available for grant or issuance has been acquired through exercise of
options or grants of shares, or until February 6, 2022, whichever is earlier. The 2012 Plan may also be terminated in the event
of certain corporate transactions such as a merger or consolidation or the sale, transfer or other disposition of all or substantially
all of our assets.
January 29, 2013, our Board of Directors conditionally approved the adoption of an annex (the “Annex”) to the 2012
Plan. Approval of the Annex by our Board of Directors was contingent upon the following: 1) 30 days elapsing since approval of
the Annex by the Board of Directors, and 2) filing with Israeli income tax authorities (the “Tax Authorities”). On
February 7, 2013, the Annex was filed with the Tax Authorities and on March 8, 2013, the Annex became effective.
Annex applies only to grantees who are residents of the State of Israel at the date of grant or those who are deemed to be residents
of the State of Israel for the payment of tax at the date of grant. U.S. tax rules and regulations will not apply to any grants
to a grantee who is a resident of the State of Israel at the date of grant or those who are deemed to be residents of the State
of Israel for the payment of tax at the date of grant.
purpose of the approval and adoption of the Annex is to harmonize the terms and conditions of the 2012 Plan with applicable Israeli
law and provide specific provisions regarding optionees who are subject to Section 102(a) of the Israeli Income Tax Ordinance
(New Version), 5721-1961 (the “Ordinance”). The Annex is intended to promote our interests by providing present and
future officers, other employees (including directors who are also our employees) and consultants with an incentive to enter into
and continue in our employ and to acquire a proprietary interest in our long-term success. Our Board of Directors shall have the
authority to determine additional persons which will be granted rights under the Annex.
to the Annex, our Board of Directors is authorized to grant stock options to persons subject to the Ordinance. Our Board of Directors
may grant to employees, officers, and directors options under Section 102 of the Ordinance, or 102 Options, and to consultants
and other service providers options under Section 3(i) of the Ordinance, or 3(i) Options. Our Board of Directors may designate
102 Options as “Approved 102 Options,” for which the options and shares upon exercise must be held in trust and granted
through a trustee, and as “Unapproved 102 Options,” for which the options and shares upon exercise do not have to
be held in trust. As described further below, the type of option and duration of time the option and shares upon exercise are
held in trust will determine the tax consequences to the participant. Of the Approved 102 Options, our Board of Directors may
grant options as “Work Income Options,” for which the options and shares upon exercise must be held in trust for 12
months from the date of grant, or as “Capital Gain Options,” for which the options and shares upon exercise must be
held in trust for 24 months from the date of grant. If the requirements of the Approved 102 Options are not met, the options are
regarded as Unapproved 102 Options. 3(i) Options and the shares upon exercise may be held in trust as well, depending upon the
agreement between our Board of Directors, optionee, and the trustee of the trust. Approved 102 Options which have been granted
as “Capital Gains Options” enable the optionee to pay capital gains tax on such option provided the terms of the grant
and Section 102 of the Ordinance have been met whilst all other option grants under the Annex are treated as regular income and
are subject to the taxation applicable thereto. The trustee appointed under the Annex is required to qualify as a trustee under
Section 102 of the Ordinance and shall hold any options granted under the Annex in trust for the respective holding periods as
designated under the Annex and Section 102 of the Ordinance. The grant of options under the Annex requires the delivery of a grant
notification letter to each optionee in which all the relevant terms and conditions of such grant are set out. The grant notification
letter may include additional matters relating to the vesting of the options, exercise periods, events of termination of employment,
etc. The Annex sets out that for as long as options or shares purchased pursuant to thereto are held by the trustee on behalf
of the optionee, all rights of the optionee over the shares are personal, cannot be transferred, assigned, pledged or mortgaged,
other than by will or laws of descent and distribution. The Annex shall be governed by and construed and enforced in accordance
with the laws of the State of Delaware.
following table summarizes information as of the close of business on December 31, 2017 concerning the 2012 Plan and other options
||Weighted-average exercise price of outstanding options |
||Securities remaining available for future issuance under equity compensation plans (excluding securities reflected in column (a))|
|Equity compensation plans approved by security holders||
|| ||4,896|| ||
|| ||191.04|| ||
|| ||40,474|| |
|Equity compensation plans not approved by security holders||
|| ||-|| ||
|| ||-|| ||
|| ||-|| |
|| ||4,896|| ||
|| ||191.04|| ||
|| ||40,474|| |
Stock Incentive Plan
February 22, 2018, the Board of Directors approved the adoption of the 2018 Stock Incentive Plan (the “2018 Plan”),
including an Israeli annex to comply with Israeli law, in particular the provisions of section 102 of the Israeli Income Tax Ordinance.
Under the 2018 Plan, we may grant our employees, directors, consultants and/or contractors stock options, shares of Common Stock,
restricted stock and restricted stock units of our company. The Board of Directors is currently serving as the administrator of
the 2018 Plan, although the 2018 Plan allows for the administrator to be a committee of the Board of Directors appointed by the
Board of Directors for the purpose of the administration of the 2018 Plan. Each stock option granted is exercisable, unless otherwise
determined by the administrator, in twelve equal installments over the three year period from the date of grant. Unless otherwise
determined by the administrator, the term of each award will be seven years. The exercise price per share subject to each option
will be determined by the administrator, subject to applicable laws and to guidelines adopted by the Board of Directors from time
to time. In the event the exercise price is not determined by the administrator, the exercise price of an option will be equal
to the closing stock price of the Common Stock on the last trading day prior to the date of grant. Upon the adoption of the 2018
Plan, the Board of Directors reserved for issuance 435,052 shares of Common Stock.
connection with the Merger and for no consideration, each of the holders of outstanding equity awards of Wize Israel, subject
to and effective upon the closing of the Merger, agreed to cancel any and all options or other rights to purchase Wize Israel’s
shares that were not exercised at least seven business days prior to the closing of the Merger, such that no equity awards of
Wize Israel were outstanding upon the closing of the Merger.
13. CERTAIN RELATIONSHIPS AND RELATED TRANSACTIONS, DIRECTOR INDEPENDENCE.
below are the transactions and series of similar transactions since January 1, 2017 to which we were a party in which:
amounts involved exceeded the lesser of $120,000 or one percent of our total assets at year end for the last two completed
fiscal years; and|
of the directors, executive officers, holders of more than 5% of our share capital, or any member of their respective immediate
family had or will have a direct or indirect material interest.|
Israel Loan Agreements and the 2017 Private Placement
January 15, 2017, Wize Israel entered into the 2017 Loan Agreement with Ridge, and, by way of entering into assignments and assumption
agreements following such date, also with Rimon Gold and Fisher. Prior to entering into the 2017 Loan Agreement, Wize Israel entered
into the Ridge Interim Loans with Ridge. On June 23, 2017, Wize Israel entered into the 2017 PIPE Agreements with each of Peretz,
Zarachia, Sadan and Rubini. Each of Ridge, Rimon Gold, Fisher, Peretz, Zarachia, Sadan and Rubini beneficially held more than
5% of the share capital of Wize Israel as a result of such transactions.
more information relating to the Convertible Loans, the agreements relating thereto and the 2017 PIPE Agreements, please see Item
7 - “MANAGEMENT’S DISCUSSION AND ANALYSIS OF FINANCIAL CONDITION AND RESULTS OF OPERATIONS,” beginning on page
62 of this Annual Report.
with Executive Officers and Directors
with Wize Israel’s Directors and Executive Officers.
Noam Danenberg, our Chief Operating Officer and Wize Israel’s strategic advisor, is also the son-in-law of Mrs. Hanna Harpaz,
who owns 49% of Ridge.
Israel has entered into employment, services and other agreements with certain of its directors and executive officers. For more
information regarding these other agreements entered into by Wize Israel with certain of its executive officers, please see Item
11 - “EXECUTIVE COMPENSATION — Executive Employment Agreements,” beginning on page 79 of this Annual Report,
Item 11 - “EXECUTIVE COMPENSATION — Compensation of Directors -- Services Agreement with Ron Mayron,”
beginning on page 81 of this Annual Report, and Item 11 - “EXECUTIVE COMPENSATION — Compensation of Directors
-- Finder’s Fee Agreement with Joseph Zarzewsky,” on page 82 of this Annual Report.
and Undertaking Agreement
with the execution of the Merger Agreement and as contemplated therein, Can-Fite entered into a Voting and Undertaking Agreement
with us and Wize Israel (the “Voting and Undertaking Agreement”), pursuant to which Can-Fite agreed to vote our shares
held by it in favor of approving the matters on the agenda of the 2017 Annual Meeting and against any actions that could adversely
affect the consummation of the Merger. In addition, the Voting and Undertaking Agreement placed certain restrictions on the transfer
of our shares held by Can-Fite. Furthermore, Can-Fite agreed to indemnify us and Wize Israel with respect to certain of our liabilities
occurring in the period up to the closing of the Merger but excluding certain liabilities in respect of any legal proceedings
arising out of or related to the transactions contemplated by the Merger Agreement.
November 21, 2011, we entered into the Can-Fite License Agreement with Eyefite and Can-Fite. As a condition to closing of the
Merger, the Can-Fite License Agreement was required to be terminated pursuant to a Termination of License Agreement, which was
entered into by Can-Fite and Eyefite on the Closing Date. On November 21, 2011, EyeFite and Can-Fite entered into the Can-Fite
Services Agreement. As a condition to closing of the Merger, the Can-Fite Services Agreement was required to be terminated pursuant
to a Termination of Services Agreement, which was entered into by Can-Fite, Eyefite and us on the Closing Date. Pursuant to the
Termination of Services Agreement, Can-Fite waived any and all payments owed to it by us under the Services Agreement and outstanding
as of the Effective Date so that any and all such amounts were waived and cancelled.
was our majority stockholder prior to the Effective Time. Dr. Fishman, our former Chief Executive Officer and Chairman, is also
the Chief Executive Officer of Can-Fite and Messrs. Cohn and Regev, both our former directors, are also directors of Can-Fite.
Itay Weinstein, our former Chief Financial Officer, is the controller of Can-Fite.
Item 10 – “DIRECTORS, EXECUTIVE OFFICERS AND CORPORATE GOVERNANCE –Director Independence,” beginning on
page 75 of this Annual Report.
for Approval of Related Party Transactions
Board is charged with reviewing and approving all potential related party transactions. All such related party transactions
must then be reported under applicable SEC rules. We have not adopted other procedures for review, or standards for approval,
of such transactions, but instead review them on a case-by-case basis.
14. PRINCIPAL ACCOUNTING FEES AND SERVICES.
February 15, 2018, the Company dismissed Kost Forer Gabbay & Kasierer, a member of Ernst & Young Global (“EY”)
as the Company’s independent registered public accounting firm and engaged Fahn Kanne & Co. Grant Thornton Israel (“Grant
Thornton”) as its new independent registered public accounting firm. The Board of Directors made the decision to dismiss
EY and engage Grant Thornton, the independent registered public accounting firm of Wize Pharma Ltd., the Company’s wholly
of the reports of EY on the Company’s financial statements for either of the past two years or subsequent interim period
contained an adverse opinion or disclaimer of opinion, or was qualified or modified as to uncertainty, audit scope or accounting
principles, except that EY’s report on the Company’s audited financial statements for the years ended December 31,
2016 and 2015 included an explanatory paragraph regarding substantial doubt about the Company’s ability to continue as a
the Company’s two most recent years ended December 31, 2016 and 2015, and the subsequent interim periods preceding their
dismissal, there were (i) no disagreements with EY, whether or not resolved, on any matter of accounting principles or practices,
financial statement disclosure, or auditing scope or procedure, which, if not resolved to the satisfaction of EY, would have caused
it to make reference to the subject matter of the disagreement in connection with its report on the Company’s financial
statements and (ii) no reportable events (as described in paragraph 304(a)(1)(v)) of Regulation S-K).
the two most recent fiscal years and the interim periods preceding the engagement, and through the date of this Report, neither
the Company nor anyone on its behalf has previously consulted with Grant Thornton regarding either (a) the application of accounting
principles to a specified transaction, either completed or proposed; or the type of audit opinion that might be rendered on the
Company’s financial statements, and neither a written report was provided nor oral advice was provided to the Company that
concluded was an important factor considered by the Company in reaching a decision as to the accounting, auditing or financial
reporting issue; or (b) any matter that was either the subject of a disagreement (as defined in paragraph 304(a)(1)(iv) of Regulation
S-K and the related instructions thereto) or a reportable event (as described in paragraph 304(a)(1)(v)) of Regulation S-K).
following table shows the fees paid or accrued by us for the audit and other services provided by Grant Thornton and EY for 2017
|Audit Fees - Grant Thornton (1)
|Audit Fees - EY (1)