Cynapsus Announces Positive Results of CTH-104 Clinical Study of
APL-130277 for Parkinson's Disease
TORONTO, ONTARIO--(Marketwired - Apr 24, 2014) - Cynapsus
Therapeutics Inc. (TSX-VENTURE:CTH)(OTCQX:CYNAF), a specialty
pharmaceutical company, today announced positive data from its
recently completed CTH-104 healthy volunteer pilot study of a
single 25mg sublingual strip (APL-130277) dose of apomorphine.
APL-130277 is an easy-to-administer, fast-acting reformulation of
apomorphine, which is the only approved drug in the United States,
Europe, Japan and other countries for the acute rescue of "off"
motor symptoms of Parkinson's disease.
Mr. Anthony Giovinazzo, President and CEO of Cynapsus commented,
"The results from the CTH-104 study in human healthy volunteers are
very important as we move forward with testing APL-130277 in
Parkinson's patients. Not only have we demonstrated dose
proportionality of the doses tested in CTH-103 (10mg and 15mg) and
CTH-104 (25mg), but we have demonstrated in CTH-104 that the 25mg
dose is sustained over an extended period of time (162 minutes)
above the minimal efficacious plasma concentration of apomorphine
(approximately 3ng/ml), which is believed to be a level
demonstrating symptomatic relief of "off" symptoms. Importantly, we
believe we are closer to our goal of being able to provide
neurologists and movement disorder specialists with a range of
doses that are needed to treat their patients experiencing "off"
episodes. We look forward to moving on to our next clinical study
(CTH-105) in patients with Parkinson's disease who are naïve to the
use of apomorphine and who experience at least one daily "off"
episode."
Dr. Albert Agro, Chief Medical Officer at Cynapsus, also
commented: "The pharmacokinetic data we have gathered to date not
only supports delivery of our formulation by the sublingual route,
but also gives us confidence that our formulation may offer several
clinically important benefits. We look forward to demonstrating the
effectiveness of our drug in Parkinson's patients."
CTH-104 Key Findings
The CTH-104 study was a single dose, single arm,
placebo-controlled, healthy volunteer pharmacokinetic study, which
was designed to examine the pharmacokinetic profile of the 25mg
dose of APL-130277. In total, 13 subjects completed the study (11
active and 2 placebo). The following are the key findings of the
CTH-104 study, which are also compared to the results of the
CTH-103 study (See the Corporation's January 13, 2014 Press
Release):
- Dose Proportionality. A higher blood concentration of
apomorphine was achieved when comparing the 25mg dose of APL-130277
used in CTH-104 to the 10mg and 15mg doses used in the CTH-103
study. Importantly, dose proportionality was achieved when
comparing the maximum concentration achieved (Cmax) and the area
under the curve (AUC). Dose proportionality allows clinicians to
know that increasing the dose of the drug will increase the
patients' exposure to the drug in a predictable way.
- Time to Maximum Concentration (Tmax). The Tmax for the 25mg
dose of APL-130277 was approximately 40 minutes, which was similar
for the 10mg and 15mg doses of APL-130277. The rapid uptake of
apomorphine in the APL-130277 strips is comparable to that
described in the Apokyn® label (i.e. between 10 and 60
minutes).
- Maximum Concentration (Cmax). The mean Cmax of the 25mg dose of
APL-130277 was greater than the Cmax of the 10mg and 15mg doses, as
expected. The pharmacokinetic profiles of all three doses of
APL-130277 showed more rounded curves, as compared to the sharper
peaks seen following subcutaneous injections of apomorphine.
- Minimum Efficacious Blood Level (Extrapolated Time-to-On). The
minimal efficacious plasma concentration of apomorphine that
demonstrates symptomatic relief of "off" symptoms in patients with
Parkinson's disease ranges from 1.5ng/ml to 4.5ng/ml. The 25mg dose
of APL-130277 achieved within 8 minutes an average minimum
threshold concentration of 3ng/ml. The time to reach 3ng/ml in 10mg
and 15mg doses of APL-130277 was approximately 13 minutes and 10
minutes, respectively.
- Duration Above Minimum Efficacious Blood Level (Extrapolated
Time On). The average duration above 3ng/ml was 162 minutes for the
25mg dose of APL-130277. This compares favourably to the 10mg and
15mg doses of APL-130277 where the average duration above 3ng/ml
was 66 minutes and 129 minutes, respectively. The extended duration
of apomorphine plasma levels above blood concentration associated
with "on" in Parkinson's patients (approximately 3ng/ml) may
provide a longer clinical benefit to patients than following the
subcutaneous injection of apomorphine.
- No Dose Limiting Side Effects. The side effects observed in the
CTH-104 study were mild to moderate and were not defined to be dose
limiting. The onset of adverse events was consistently between 15
minutes and 30 minutes after dosing. The most common adverse events
were sleepiness, dizziness and nausea.
*Note: The CTH-103 study was designed as a three-dose (10mg,
15mg and 25mg) active comparator, placebo-controlled, randomized
cross-over trial to examine the pharmacokinetic profile of
sublingual administered APL-130277 compared to (2mg, 3mg and 4mg)
subcutaneous injections of apomorphine in healthy volunteers (See
January 13, 2014 Press Release). The 10mg and 15mg APL-130277
sublingual thin film strips were crossed over to 2mg and 3mg
subcutaneous injections, with N=15 and N=14 for the two cohorts,
respectively. The intent in the CTH-103 study for the third cohort
was to compare the 25mg sublingual thin film strip (APL-130277) to
the 4mg subcutaneous injection, but this third cohort could not be
dosed due to the dose-limiting adverse events experienced with the
3mg subcutaneous injection. The 15mg APL-130277 side effects were
mild-to-moderate and not dose limiting. As a result, the
Corporation completed the CTH-104 study, a single arm, healthy
volunteer pharmacokinetic study to look at the 25mg APL-130277
sublingual strip (without a crossover to the injection).
Critical Next Steps
For development of APL-130277 in the United States, the
Corporation will follow the 505(b)(2) regulatory pathway.
Specifically, the Corporation is pursuing the reformulation of
apomorphine from a subcutaneous injection to a convenient,
tolerable and safe sublingual thin film strip. The drug being
delivered (apomorphine) is identical to the drug used in the
injection, and its use will be intended as an acute rescue therapy
for Parkinson's patients experiencing acute, intermittent
hypomobility (i.e. "off" episodes) associated with advanced
Parkinson's disease, which is the description of the use of
apomorphine in the current U.S. approved label.
The 505(b)(2) pathway will require that the Corporation provide
statistically sufficient clinical evidence that Parkinson's
patients experience management of their "off" episodes, as a result
of delivery of apomorphine via the sublingual thin film strip
route. The primary end point will be based on changes in the
Unified Parkinson's Disease Rating Scale Part III (UPDRS III)
movement score. In addition, the Corporation will be required to
provide in a separate study, statistically sufficient clinical
evidence that administering apomorphine via a sublingual thin film
route results in Parkinson's patients experiencing low to no oral
irritation as a result of multiple daily exposures to the drug for
an extended period.
To achieve this, the Corporation currently expects to complete
the following clinical studies:
- CTH-105 Pilot Study. A pilot study in patients with Parkinson's
disease who are naïve to the use of apomorphine and who experience
at least one daily "off" episode with a total duration of "off" in
any 24-hour period of at least 2 hours. This study is planned to
examine the effect of APL-130277 on relieving "off" episodes over a
single day with a dose-titration used to determine dose strengths
necessary for future clinical development.
- CTH-200 Bridging Study. A single dose, crossover comparative
bioavailability and PK study in healthy volunteers. This study is
designed to provide the clinical "bridge" to the FDA's finding of
safety and efficacy for the Reference Listed Drug (s.c.
Apomorphine).
- CTH-300a Efficacy Study in apomorphine naïve patients. A
double-blind, placebo-controlled, parallel-design study with
Parkinson's patients who have at least one "off" episode every 24
hours, with total "off" time of at least 2 hours. The primary end
point will be the change in the UPDRS III score.
- CTH-300b Efficacy Study in apomorphine experienced patients. A
double blind, placebo controlled, crossover-designed study with
Parkinson's patients who are presently controlled with the use of
apomorphine. The primary end point will be the change in the UPDRS
III score. Upon successful completion of CTH-300a and CTH-300b, the
Corporation will provide the results to the FDA and request a
meeting to seek final guidance for the design of Safety Study
(CTH-301).
- CTH-301 Safety Study. A long-term safety study in apomorphine
naïve Parkinson's patients who have at least one "off" episode
every 24 hours, with total "off" time of at least 2 hours. The
study will specifically look at the safety and tolerability of the
new delivery route over a minimum period of 16 weeks.
The above clinical development plan has been vetted with both
clinical experts and regulatory consultants who have expertise in
overseeing FDA 505(b)(2) submissions to the Agency.
In parallel to the studies described above, the Corporation will
be performing the necessary scale-up, process validation and
stability as part of the Chemistry, Manufacturing and Controls
("CMC") requirements for the filing of the NDA. Accordingly, all
development will be performed according to current Good
Manufacturing Practices ("cGMP") methodology.
Upon completion of the efficacy and safety studies, as well as
the CMC section, the Corporation expects to begin preparation of a
FDA 505(b)(2) NDA in 2016.
About Apomorphine
Apomorphine, a potent dopamine agonist, is the only drug
approved specifically for the treatment of acute motor
fluctuations/hypomobility (freezing or "off" episodes) in patients
with advanced Parkinson's disease. Presently, apomorphine is
administered by intermittent subcutaneous injection usually via a
pre-filled injection pen, or, in some cases outside the United
States, by continuous infusion pump. Drawbacks associated with
subcutaneous injection therapy for patients and caregivers include
aversion to needles, the need for multiple injections, which can be
painful and are often associated with irritation and inflammation
at the injection site, and the requirement for a degree of manual
dexterity that some Parkinson's patients find difficult.
About Cynapsus Therapeutics
Cynapsus is a specialty pharmaceutical company developing a
convenient and easy to use sublingual (oral) thin film strip for
the acute rescue of "off" motor symptoms of Parkinson's disease.
Cynapsus' drug candidate, APL-130277, is an easy-to-administer,
fast-acting reformulation of apomorphine, which is the only
approved drug (in the United States, Europe, Japan and other
countries) to rescue patients from "off" episodes. Cynapsus is
focused on maximizing the value of APL-130277 by completing pivotal
studies in advance of a New Drug Application ("NDA") expected to be
submitted in 2016.
Over one million people in the U.S. and an estimated 4 to 6
million people globally suffer from Parkinson's disease.
Parkinson's disease is a chronic and progressive neurodegenerative
disease that impacts motor activity, and its prevalence is
increasing with the aging of the population. Based on a recent
study and the results of the Corporation's Global 500 Neurologists
Survey, it is estimated that between 25 percent and 50 percent of
patients experience "off" episodes in which they have impaired
movement or speaking capabilities. Current medications only control
the disease's symptoms, and most drugs become less effective over
time as the disease progresses.
More information about Cynapsus (TSX-VENTURE:CTH)(OTCQX:CYNAF)
is available at www.cynapsus.ca and at the System for Electronic
Document Analysis and Retrieval (SEDAR) at www.sedar.com.
Forward-Looking Statements
This announcement contains "forward-looking statements" within
the meaning of applicable securities laws. Generally, these
forward-looking statements can be identified by the use of
forward-looking terminology such as "plans", "expects" or "does not
expect", "is expected", "budget", "scheduled", "estimates",
"forecasts", "intends", "anticipates" or "does not anticipate", or
"believes" or variations of such words and phrases or state that
certain actions, events or results "may", "could", "would", "might"
or "will be taken", "occur" or "be achieved". Forward-looking
statements are subject to known and unknown risks, uncertainties
and other factors that may cause the actual results, level of
activity, performance or achievements of Cynapsus to be materially
different from those expressed or implied by such forward-looking
statements, including but not limited to those risks and
uncertainties relating to Cynapsus' business disclosed under the
heading "Risk Factors" in its March 26, 2014, Annual Information
Form and its other filings with the various Canadian securities
regulators which are available online at www.sedar.com. Although
Cynapsus has attempted to identify important factors that could
cause actual results to differ materially from those contained in
forward-looking statements, there may be other factors that cause
results not to be as anticipated, estimated or intended. There can
be no assurance that such statements will prove to be accurate, as
actual results and future events could differ materially from those
anticipated in such statements. Accordingly, readers should not
place undue reliance on forward-looking statements. Cynapsus does
not undertake to update any forward-looking statements, except in
accordance with applicable securities laws.
Neither the TSX Venture Exchange nor the OTCQX International has
passed upon the merits of the Offering or approved or disapproved
the contents of this press release.
Cynapsus TherapeuticsAnthony GiovinazzoPresident and CEO(416)
703-2449 x225ajg@cynapsus.caCynapsus TherapeuticsAndrew WilliamsCOO
& CFO(416) 703-2449
x253awilliams@cynapsus.cawww.cynapsus.ca
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