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8-K - FORM 8-K - NOVELION THERAPEUTICS INC. | c97600e8vk.htm |
EX-99.1 - EXHIBIT 99.1 - NOVELION THERAPEUTICS INC. | c97600exv99w1.htm |
Exhibit 99.2
news release
QLT ANNOUNCES PHASE II CLINICAL TRIAL RESULTS AND DEVELOPMENT PLANS
FOR THE PUNCTAL PLUG DELIVERY SYSTEM
FOR THE PUNCTAL PLUG DELIVERY SYSTEM
| 90-Day Retention Rate of 81% for Latest Punctal Plug Prototype Device |
|
| No Dose Response Seen with Higher Doses in Phase II Clinical Studies |
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| Expand Development Plans of the Punctal Plug Delivery System in Allergic Conjunctivitis |
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| Clinical Results and Plans for Expansion to be Discussed During Todays Conference Call |
For Immediate Release | March 10, 2010 |
VANCOUVER, CANADAQLT Inc. (NASDAQ: QLTI; TSX: QLT) (QLT or the Company) today announced
results from Phase II clinical trials and a device study for the punctal plug delivery system
(PPDS). These studies are part of a development program that is being conducted by QLTs
wholly-owned subsidiary, QLT Plug Delivery, Inc. QLT also announced its plans to expand the program
to evaluate a second drug for a new target indication.
Device Retention and New Developments
Recent clinical data on the third-generation punctal plug designs demonstrate a retention rate of
81%, based on available data from 185 eyes with 12 weeks of follow-up. Retention data are derived
from a study of healthy volunteers testing several punctal plug prototype designs and from Phase II
studies of the latanoprost punctal plug delivery system (L-PPDS) in patients with open-angle
glaucoma (OAG) or ocular hypertension (OH), in which the third-generation prototypes were used.
Punctal plug designs are continuing to be refined to maximize retention rates. The Company will
provide an update on retention rate results by year-end.
In parallel with the punctal plug device refinements, additional activities are focused on
optimizing an insertion tool and development of a simple home-use detection system that would allow
patients to confirm the presence of the punctal plugs.
L-PPDS Phase II Dosing Trials
The concurrent open-label, multicenter Phase II trials of the punctal plugs investigating the use
of higher doses of latanoprost from previous studies did not demonstrate a dose-response. These
Phase II clinical trials have evaluated the safety, efficacy, and dosing for L-PPDS treatment of
subjects with OAG and OH. L-PPDS containing latanoprost concentrations of 44 µg, 81 µg, and two
different 95 µg formulations have been evaluated. The 95 µg formulations were developed to deliver
different average daily doses. The third-generation punctal plug designs were used with the 81 µg
and both 95 µg L-PPDS formulations.
Page 1 of 5
Range of the mean intraocular pressure (IOP) change from baseline (mmHg) in the Phase II studies:
Latanoprost Concentration in L-PPDS | ||||||||||||||||
44 µg | 81 µg | 95 µg (A) | 95 µg (B)* | |||||||||||||
Number of Subjects |
N=57 | N=53 | N=42 | N=39 | ||||||||||||
Mean IOP Baseline Value
(mmHg) |
24.5 | 25.4 | 25.1 | 25.0 | ||||||||||||
Range of Mean IOP
Change from Baseline: Weeks 1 to 6 (mmHg) |
-3.3 to -3.6 | -1.9 to -3.4 | -3.4 to -4.1 | -3.0 to -4.7 | ||||||||||||
Status of Phase II Trial |
Complete | Complete | Ongoing to 12 weeks follow-up | Ongoing to 12 weeks follow-up | ||||||||||||
Equivalent Number of
latanoprost Eye Drops
(% of Amount in Eye
Drops over 3 Months) |
29 (32 | %) | 54 (60 | %) | 63 (70 | %) | 63 (70 | %) |
* | The B formulation was designed to deliver a higher average daily dose than the A
formulation. |
The objective of these trials was to identify
formulations that achieve a ≥5 mmHg drop in mean IOP.
Because a dose-response is not evident across all L-PPDS formulations tested, new nonclinical
research efforts are underway to evaluate alternative approaches to improving the delivery of
latanoprost to its target receptors inside the eye. The Company will provide an update on the
status of its efforts in the fourth quarter of this year.
I am pleased with the improvements we have made in the punctal plug retention rate. We continue to
work to maximize our retention rates and to explore what retention rate may be acceptable for a
commercial product, said Bob Butchofsky, President and Chief Executive Officer of QLT. Although
we did not see the dose response in our on-going L-PPDS studies, we now know that there are
multiple factors that affect drug delivery from a punctal plug and our research efforts for the
latanoprost PPDS will be focused on addressing those factors. Building on that knowledge, the next
step for this platform technology will be a clinical trial with olopatadine, a compound which
targets ocular tissue on the surface of the eye.
Expansion of Punctal Plug Delivery Platform to Olopatadine and Allergic Conjunctivitis
The second drug candidate selected for the punctal plug delivery platform is olopatadine, an
anti-allergy drug. Olopatadine is an active pharmaceutical ingredient that has been approved by the
U.S. Food and Drug Administration in an eye drop dosage form for the treatment of the signs and
symptoms of allergic conjunctivitis. The PPDS platform may be well-suited for olopatadine delivery
to the surface of the eye. Furthermore, retention rates of the third-generation punctal plug over 6
weeks (the intended duration of sustained delivery for this product) are greater than 85%. A
short-term, proof-of-concept study to evaluate the preliminary efficacy and safety of a
sustained-release olopatadine PPDS for allergic conjunctivitis is expected to begin in the second
half of 2010 with results expected by year-end.
Page 2 of 5
About the Device Study (Punctal Plug Prototype Designs)
This study is an ongoing, device, open-label, multicenter study conducted to investigate the
safety, tolerability, comfort, ease of handling and insertion/removal, and retention of punctal
plug prototype designs, in healthy subjects. More than 800 healthy volunteers have been fitted with a punctal plug
in each eye and wear the devices for up to 12 weeks. Enrollment is ongoing. Interim analyses show
that the third-generation punctal plug designs have been well tolerated. The most frequently
reported adverse device events for subjects fitted with the third generation punctal plug (without
drug) have been eye itching (6.5%); increased lacrimation and ocular discomfort (3.7% for each
event); and conjunctival hyperemia, conjunctival edema, foreign body sensation in eyes, and eyelid
edema (2.8% for each event). Comfort scores for the third-generation punctal plugs are greater than
90 out of 100 on a scale where 100 points equals no awareness.
Prototype punctal plug designs continue to be refined and evaluated to further improve retention
rates and selection of the final design will converge with the identification of a dose formulation
that is to be taken into later-stage clinical trials.
About the 44-µg and 81-µg Phase II Study
This completed Phase II, open-label, multicenter study included two cohorts and was conducted to
investigate the safety and preliminary efficacy of L-PPDS containing either 44 µg (first cohort) or
81 µg (second cohort) of latanoprost, a prostaglandin analogue, in subjects with OAG or OH over a
six-week period. A total of 113 subjects diagnosed with OAG/OH were enrolled: 60 into the 44 µg
cohort and 53 into the 81 µg cohort. The mean age was 65 years and mean baseline IOP was 24.9 ± 2.2
mmHg. In cohort 1 (44 µg), 46 subjects (77%) completed all six weeks of treatment and had an IOP
measurement at Week 6, while 14 subjects (23%) discontinued L-PPDS treatment early primarily due to
either loss of L-PPDS or inadequate IOP control. In cohort 2 (81 µg), a higher percentage of
subjects completed the six week treatment period and had an IOP measurement at Week 6 (50 subjects,
94%). Three subjects (6%) discontinued L-PPDS treatment early primarily due to inadequate IOP
control.
The L-PPDS was well-tolerated over the testing period. The overall adverse events range from 1.7%
to 11.7% for the 44 µg L-PPDS (cohort 1) and from 1.9% to 22.6% for the 81 µg L-PPDS (cohort 2).
Eye itching (commonly seen with initial punctal plug wear) and increased tearing were the most
common adverse events (11.7% and 10.0%, respectively, in cohort 1, and 20.8% and 22.6%,
respectively, in cohort 2). Foreign body sensation and superficial punctate keratitis were reported
in 6.7% and 5.0%, respectively, of cohort 1 subjects and in 7.5% (for each event) of cohort 2
subjects. In general, adverse event incidence was higher for the 81 µg L-PPDS (cohort 2) than for
the 44 µg L-PPDS (cohort 1). Conjunctival hyperemia and ocular hyperemia were reported exclusively
in cohort 2 (5.3% and 1.8% of all subjects, respectively), as well as eyelid erythema (2.7%). Most
events were mild in intensity in both cohorts (41 of 58 events in cohort 1, and 90 of 132 events in
cohort 2). Despite the higher incidence of adverse events in cohort 2 (81 µg L-PPDS), comfort and
tearing scores were comparable between cohorts 1 and 2 over the six-week study period. L-PPDS
comfort combined grades of no awareness and mild awareness ranged from 88% to 98% in cohort 1
and from 94% to 98% in cohort 2 over the six weeks. Tearing combined grades of none and
occasional ranged from 85% to 96% in cohort 1 and from 81% to 89% in cohort 2 over six weeks.
About the 95-µg Phase II Study
This study is an ongoing, Phase II, open-label, multicenter study conducted to investigate the
safety and preliminary efficacy of two different formulations of L-PPDS containing 95-µg
latanoprost, in subjects with OAG or OH over a 12-week period. Eighty-one subjects diagnosed with
OAG/OH have been enrolled. The mean age is 63 years and mean baseline IOP is 25.0 ± 2.4 mmHg.
The L-PPDS has been well-tolerated over the testing period. Based on preliminary data of 70
subjects (86%) who have completed 6 weeks of follow-up, the overall incidence of adverse events
ranges from 1.2% to 9.9%. The most common adverse events are conjunctival hyperemia (9.9%), eyelid
itching (8.6%), and eye itching (6.2%). At Week 6, 97% of subjects rated L-PPDS comfort as no awareness
or mild awareness, and 97% of subjects rated tearing as none or occasional.
Page 3 of 5
About the Latanoprost Punctal Plug Delivery System (L-PPDS)
The L-PPDS is a novel, sustained and controlled release drug delivery system that utilizes the
puncta to house a drug-eluting device. The L-PPDS is currently being investigated as a treatment
for OAG and OH patients to particularly address patient non-compliance issues. The punctal plug
delivery system is a minimally invasive drug delivery system that is being developed with a goal of
enabling delivery of a variety of drugs to the eye over time through sustained release to the tear
film.
About Prostaglandins
Prostaglandins represent the largest segment of the U.S. glaucoma market. Latanoprost is an active
ingredient that has been approved by the Food and Drug Administration for reducing elevated
intraocular pressure in patients with OAG or OH and is marketed under the trade name Xalatan® in
the U.S. Latanoprost is the most-prescribed glaucoma medicine in the world and had franchise sales
in 2009 of approximately $1.75 billion (Pfizer).
About Olopatadine
Olopatadine blocks the release of histamine from mast cells. Olopatadine is an active
pharmaceutical ingredient that has been approved by the Food and Drug Administration for the
treatment of the signs and symptoms of allergic conjunctivitis and is marketed under the trade
names Pataday and Patanol® in the U.S. (Alcon). U.S. sales of olopatadine were more
than $380 million in 2009.
About Allergic Conjunctivitis
Over 50 million people in the U.S. suffer from allergic diseases, and it is estimated that 40%-60%
of the allergic population suffer from ocular symptoms. In allergic conjunctivitis, patients suffer
from localized itchiness, redness, tearing, and swelling of the eyelid upon exposure of the eye to
airborne allergens, such as pollen, mold, dust mites, or animal dander. In severe cases, chronic
scratching of the eyes due to allergic symptoms may be associated with corneal or conjunctival
scarring, growth of blood vessels in the cornea, and changes in visual acuity.
Conference call information
QLT Inc. will hold an investor conference call to discuss 2009 results and the PPDS study results
on Wednesday, March 10, 2010 at 8:30 a.m. ET (5:30 a.m. PT). The call with slides will be broadcast
live via the Internet at www.qltinc.com. To participate on the call, please dial
1-800-319-4610 (North America) or 604-638-5340 (International) before 8:30 a.m. ET. For those
dialing in to the call, the presentation slides will be available on QLTs web site at
www.qltinc.com. A replay of the call will be available via the Internet and also via telephone at
1-800-319-6413 (North America) or 604-638-9010 (International), access code 7157, followed by the
# sign.
About QLT
QLT Inc. is a biotechnology company dedicated to the development and commercialization of
innovative therapies for the eye. We are focused on our commercial
product Visudyne® for
the treatment of wet-AMD, and the development of drugs to be delivered in our proprietary punctal
plug devices. For more information, visit our website at www.qltinc.com.
Page 4 of 5
QLT Inc. Media Contact:
Vancouver, Canada
Karen Peterson
Telephone: 604-707-7000 or 1-800-663-5486
kpeterson@qltinc.com
Vancouver, Canada
Karen Peterson
Telephone: 604-707-7000 or 1-800-663-5486
kpeterson@qltinc.com
The Trout Group Investor Relations Contact:
New York, USA
Christine Yang
Telephone: 646-378-2929
cyang@troutgroup.com
Or
Boston, Massachusetts, USA
Tricia Swanson
Telephone: 617-583-1306
tswanson@troutgroup.com
New York, USA
Christine Yang
Telephone: 646-378-2929
cyang@troutgroup.com
Or
Boston, Massachusetts, USA
Tricia Swanson
Telephone: 617-583-1306
tswanson@troutgroup.com
QLT Plug Delivery, Inc. is a wholly-owned subsidiary of QLT Inc.
Visudyne® is a registered trademark of Novartis AG.
Xalatan® is a registered trademark of Pfizer Health AB.
Patanol® is a registered trademark of Alcon Research, Ltd.
Pataday is a trademark of Alcon, Inc.
Visudyne® is a registered trademark of Novartis AG.
Xalatan® is a registered trademark of Pfizer Health AB.
Patanol® is a registered trademark of Alcon Research, Ltd.
Pataday is a trademark of Alcon, Inc.
QLT Inc. is listed on The NASDAQ Stock Market under the trading symbol QLTI and on The Toronto
Stock Exchange under the trading symbol QLT.
Certain statements in this press release constitute forward looking statements of QLT within the
meaning of the Private Securities Litigation Reform Act of 1995 and constitute forward looking
information within the meaning of applicable Canadian securities laws. Forward looking statements
include, but are not limited to: our clinical trial and other development plans related to device
insertion and detection, prototype designs, the L-PPDS and PPDS, including future plans to initiate
a study on olopatadine for the treatment of allergic conjunctivitis, and expectations for the
timing to commence and receive and release data from these studies; our future expectations about
our PPDS and device prototypes including the potential for the PPDS to be well-suited for
olopatadine delivery to the surface of the eye; and statements which contain language such as:
assuming, may, prospects, future, projects, believes, expects and outlook.
Forward-looking statements are predictions only which involve known and unknown risks,
uncertainties and other factors that may cause actual results to be materially different from those
expressed in such statements. Many such risks, uncertainties and other factors are taken into
account as part of our assumptions underlying these forward-looking statements and include, among
others, the following: the Companys future operating results are uncertain and likely to
fluctuate; uncertainties relating to the timing and results of the clinical development and
commercialization of our products and technologies (including Visudyne and our punctal plug
technology) and the associated costs of these programs; the timing, expense and uncertainty
associated with the regulatory approval process for products; uncertainties regarding the impact of
competitive products and pricing; risks and uncertainties associated with the safety and
effectiveness of our technology; risks and uncertainties related to the scope, validity, and
enforceability of our intellectual property rights and the impact of patents and other intellectual
property of third parties; and general economic conditions and other factors described in detail in
QLTs Annual Report on Form 10-K, Quarterly Reports on Form 10-Q and other filings with the U.S.
Securities and Exchange Commission and Canadian securities regulatory authorities. Forward looking
statements are based on the current expectations of QLT and QLT does not assume any obligation to
update such information to reflect later events or developments except as required by law.
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