SOUTH SAN FRANCISCO, CA, Mar 06, 2012 (MARKETWIRE via COMTEX) --Cytokinetics, Incorporated (NASDAQ: CYTK) announced today that the
European Medicines Agency (EMA) has granted the company's fast
skeletal muscle troponin activator CK-2017357 orphan medicinal
product designation for the treatment of amyotrophic lateral
sclerosis (ALS), also commonly known as Lou Gehrig's Disease.
CK-2017357 is the lead drug candidate that has emerged from the
Cytokinetics' skeletal sarcomere activator program. CK-2017357 is
currently the subject of an ongoing Phase II clinical development
program in patients with ALS.
Orphan medicinal product designation is adopted by the European
Commission based on an opinion that is rendered by the EMA's
Committee for Orphan Medicinal Products. Orphan medicinal product
designation is granted by the EMA to novel drugs or biologics that
are intended for the diagnosis, prevention or treatment of a
life-threatening or chronically debilitating condition affecting not
more than 5 in 10,000 persons in the European Union (EU), or for
which there is no reasonable expectation that the cost of development
and distribution of the drug will be recovered by the expected sales
under normal market conditions without the incentives provided
through this designation. The designation offers a number of
potential incentives, which may include a ten-year period of EU
marketing exclusivity from the date of marketing authorization,
EU-funded research, protocol assistance and fee reductions.
"We are pleased that the EMA has granted orphan medicinal product
status to CK-2017357 for the treatment of ALS. This designation,
along with a similar orphan drug designation already received in the
U.S. from the U.S. Food and Drug Administration, underscores the
potential for this novel drug candidate to address significant unmet
medical needs in patients suffering from this grievous and uniformly
fatal disease," said Andrew A. Wolff, M.D, Senior Vice President,
Clinical Research and Development and Chief Medical Officer of
Cytokinetics. "We look forward to working closely with the relevant
regulatory authorities, as well as with our clinical investigators
and key opinion leaders in the field of ALS, to advance this
important and promising drug candidate rapidly through the next
stages of clinical research and development."
Background on Amyotrophic Lateral Sclerosis
Amyotrophic lateral sclerosis (ALS) is a progressive
neurodegenerative disease that afflicts 20,000 to 30,000 people in
the United States and fewer than 1 in 10,000 persons in the EU.
Approximately 5,600 new cases of ALS are diagnosed each year in the
U.S., and the incidence in the U.S. is consistent on a population
basis with the EU. The average life expectancy of an ALS patient is
approximately three to five years and only 10% of patients survive
for more than 10 years. Death is usually due to respiratory failure
because of diminished strength in the skeletal muscles responsible
for breathing. Few treatment options exist for these patients,
resulting in a high unmet need for new therapeutic options to address
the symptoms and modify the disease progression of this grievous
illness.
Development Status of CK-2017357 in ALS
Cytokinetics is developing CK-2017357, a skeletal muscle activator,
as a potential treatment for diseases and conditions associated with
aging, muscle wasting or neuromuscular dysfunction. CK-2017357 is
currently the subject of a Phase II clinical development program and
has been granted orphan drug designation by the U.S. Food and Drug
Administration and orphan medicinal product designation from the
European Medicines Agency for the potential treatment of ALS, a
debilitating disease of neuromuscular impairment.
CK-2017357 demonstrated potentially clinically relevant
pharmacodynamic effects in a Phase IIa Evidence of Effect clinical
trial in ALS patients. In that trial, the single doses of CK-2017357
evaluated appeared generally well-tolerated. In addition, both
patients and investigators perceived a dose-dependent positive change
in the patients' overall status at 6 hours after dosing with
CK-2017357, based on a Global Assessment in which the patient and the
investigator each independently assessed the patient's status
compared to prior to dosing. Furthermore, there was a clear
relationship between improvements in Global Assessments and plasma
concentrations of CK-2017357. Also at this 6-hour time point, there
was a trend towards decreased muscle fatigability, as evidenced by
data from a test of sub-maximal hand-grip endurance. Data from that
clinical trial also demonstrated a statistically significant increase
in the maximum volume of air patients could inhale and exhale
(Maximum Voluntary Ventilation) at both 6 and 24 hours after 500 mg
of CK-2017357, as well as small but statistically significant
increases in maximum strength of certain muscle groups tested.
In December 2011, the company reported data from Part A of its
ongoing Phase II clinical trial (CY 4024), in which 24 ALS patients
who were not concurrently taking riluzole were randomized to one of
four different treatment groups to receive daily oral doses of
placebo or 125 mg, 250 mg, or 375 mg of CK-2017357, respectively, for
two weeks. CK-2017357 was well-tolerated by these patients at all
dose levels studied. The incidence of dizziness, the most common
adverse event, appeared dose-related but was mild in severity in all
patients who completed study drug treatment. Most reports of
dizziness began early after initiating treatment and resolved
spontaneously within the first week of treatment in all but one
patient who nevertheless completed the trial No serious adverse
events were reported. The second cohort of this clinical trial, or
Part B, is ongoing, and is intended to enroll approximately 24 ALS
patients who are concurrently taking riluzole; otherwise, Part B is
identical in design to Part A. An additional Phase II clinical trial
(CY 4025) designed to evaluate the safety and tolerability of an
ascending dose-titration regimen of CK-2017357 is also ongoing.
Cytokinetics anticipates that results from each of these two clinical
trials will be presented at the American Academy of Neurology 64th
Annual Meeting in New Orleans, LA on April 25, 2012.
Cytokinetics has met with the U.S. Food and Drug Administration's
Center for Drug Evaluation and Research's Division of Neurology
Products and with the European Medicines Agency to discuss its
progress in the development of CK-2017357 as a potential treatment
for patients with ALS and the company's plans for its further
development, including potential registration strategies.
Cytokinetics is assessing options that may enable the initiation of a
registration program for CK-2017357. Cytokinetics anticipates having
additional meetings with U.S. and European regulatory authorities
during 2012 to discuss the development of CK-2017357 as a potential
treatment for patients with ALS, including potential registration
strategies.
In July 2010, Cytokinetics was awarded a grant of approximately $2.8
million from the National Institute of Neurological Disorders and
Stroke to support research and development of CK-2017357 in
myasthenia gravis. The grant was awarded under the American Recovery
and Reinvestment Act of 2009. Cytokinetics continues to enroll and
dose patients in a Phase IIa Evidence of Effect clinical trial of
CK-2107357 in patients with generalized myasthenia gravis.
Cytokinetics anticipates that data will be available from this trial
in the first half of 2012.
Background on Cytokinetics Skeletal Muscle Contractility Program
Skeletal muscle contractility is driven by the sarcomere, the
fundamental unit of skeletal muscle contraction. The sarcomere is a
highly ordered cytoskeletal structure composed of skeletal muscle
myosin, the cytoskeletal motor that is directly responsible for
converting chemical energy into mechanical force, as well as actin,
and a set of regulatory proteins, troponins and tropomyosin, which
make the actin-myosin interaction dependent on changes in
intracellular calcium levels. Cytokinetics' skeletal muscle
contractility program is focused to the discovery and development of
small molecule skeletal sarcomere activators and leverages
Cytokinetics' expertise developed in its ongoing discovery and
development of cardiac sarcomere activators, including the cardiac
myosin activator omecamtiv mecarbil, now in Phase II clinical
development as a potential treatment for heart failure. CK-2017357, a
fast skeletal muscle troponin activator, is the lead drug candidate
from the company's skeletal muscle contractility program. CK-2017357
selectively activates the fast skeletal muscle troponin complex by
increasing its sensitivity to calcium, leading to an increase in
skeletal muscle force. This mechanism of action has demonstrated
encouraging pharmacological activity in preclinical models that may
relate to the potential treatment of diseases associated with aging,
muscle wasting or neuromuscular dysfunction. In addition, CK-2017357
has shown pharmacological activity in healthy volunteers, in patients
with amyotrophic lateral sclerosis ("ALS"), and in patients with
peripheral artery disease and claudication. The clinical effects of
muscle wasting, fatigue and loss of mobility can range from decreased
quality of life to, in some instances, life-threatening
complications. By directly improving skeletal muscle function, a
small molecule activator of the skeletal sarcomere may potentially
enhance physical performance and quality of life in patients
suffering from diseases or medical conditions characterized or
complicated by muscle weakness or wasting.
About Cytokinetics
Cytokinetics is a clinical-stage biopharmaceutical company focused on
the discovery and development of novel small molecule therapeutics
that modulate muscle function for the potential treatment of serious
diseases and medical conditions. Cytokinetics' lead drug candidate
from its cardiac muscle contractility program, omecamtiv mecarbil, is
in Phase II clinical development for the potential treatment of heart
failure. Amgen Inc. holds an exclusive license worldwide (excluding
Japan) to develop and commercialize omecamtiv mecarbil and related
compounds, subject to Cytokinetics' specified development and
commercialization participation rights. Cytokinetics is independently
developing CK-2017357, a skeletal muscle activator, as a potential
treatment for diseases and conditions associated with aging, muscle
wasting or neuromuscular dysfunction. CK-2017357 is currently the
subject of a Phase II clinical trials program and has been granted
orphan drug designation by the U.S. Food and Drug Administration and
orphan medicinal product designation by the European Medicines Agency
for the potential treatment of amyotrophic lateral sclerosis, a
debilitating disease of neuromuscular impairment in which CK-2017357
demonstrated potentially clinically relevant pharmacodynamic effects
in a Phase IIa trial. Cytokinetics is also conducting research of
compounds that inhibit smooth muscle contractility and which may be
useful as potential treatments for diseases and conditions associated
with excessive smooth muscle contraction, such as bronchoconstriction
associated with asthma and chronic obstructive pulmonary disorder
(COPD). All of these drug candidates and potential drug candidates
have arisen from Cytokinetics' research activities and are directed
towards the cytoskeleton. The cytoskeleton is a complex biological
infrastructure that plays a fundamental role within every human cell.
Additional information about Cytokinetics can be obtained at
www.cytokinetics.com.
This press release contains forward-looking statements for purposes
of the Private Securities Litigation Reform Act of 1995 (the "Act").
Cytokinetics disclaims any intent or obligation to update these
forward-looking statements, and claims the protection of the Act's
Safe Harbor for forward-looking statements. Examples of such
statements include, but are not limited to, statements relating to
Cytokinetics' and its partners' research and development activities,
including the initiation, conduct, design, scope and results of
clinical trials, including potential initiation of a clinical trial
of CK-2017357 in ALS patients that could potentially support global
registration. and the significance and utility of the results of
clinical trials and preclinical studies; the potential benefits of
orphan medicinal product designation; the potential markets for
CK-2017357; and the properties and potential benefits of CK-2017357
and Cytokinetics' other compounds. Such statements are based on
management's current expectations, but actual results may differ
materially due to various risks and uncertainties, including, but not
limited to, potential difficulties or delays in the development,
testing, regulatory approvals for trial commencement, progression or
product sale or manufacturing, or production of Cytokinetics' drug
candidates that could slow or prevent clinical development or product
approval, including risks that current and past results of clinical
trials or preclinical studies may not be indicative of future
clinical trials results, patient enrollment for or conduct of
clinical trials may be difficult or delayed, Cytokinetics' drug
candidates may have adverse side effects or inadequate therapeutic
efficacy, the U.S. FDA or foreign regulatory agencies may delay or
limit Cytokinetics' or its partners' ability to conduct clinical
trials, regulatory authorities may not grant CK-2017357 orphan
drug/medicinal product market exclusivity even if it is approved for
marketing, and Cytokinetics may be unable to obtain or maintain
patent or trade secret protection for its intellectual property;
Amgen's decisions with respect to the design, initiation, conduct,
timing and continuation of development activities for omecamtiv
mecarbil; Cytokinetics may incur unanticipated research and
development and other costs or be unable to obtain additional
financing necessary to conduct development of its products on
acceptable terms, if at all; Cytokinetics may be unable to enter into
future collaboration agreements for its drug candidates and programs
on acceptable terms, if at all; standards of care may change,
rendering Cytokinetics' drug candidates obsolete; competitive
products or alternative therapies may be developed by others for the
treatment of indications Cytokinetics' drug candidates and potential
drug candidates may target; and risks and uncertainties relating to
the timing and receipt of payments from its partners, including
milestones and royalties on future potential product sales under
Cytokinetics' collaboration agreements with such partners. For
further information regarding these and other risks related to
Cytokinetics' business, investors should consult Cytokinetics'
filings with the Securities and Exchange Commission.
Contact:
Jodi L. Goldstein
Manager, Corporate Communications and Marketing
(650) 624-3000
SOURCE: Cytokinetics, Inc.
