BRUSSELS, Dec. 8, 2014
/PRNewswire/ -- Today UCB announced the primary efficacy and
safety data from the latest Phase 3 study evaluating
brivaracetam (fixed doses of 100 and 200 mg/day with no
up-titration) as adjunctive treatment in adult epilepsy patients
with partial-onset seizures.1 This study with
brivaracetam represents the largest Phase 3 study conducted
in epilepsy patients with partial-onset seizures.
Brivaracetam is an investigational antiepileptic drug (AED)
and is not approved by any regulatory authority worldwide.
This study showed statistical significance for the two primary
endpoints (p<0.001 for brivaracetam 100 and 200 mg/day).
The primary efficacy endpoint in the US was the percent reduction
in partial-onset seizure frequency per 28 days over placebo. The
primary efficacy endpoint in the EU was the responder rate, i.e.,
the proportion of patients showing a 50% or greater reduction in
partial-onset seizure frequency. The most frequent
treatment-emergent adverse events were somnolence, dizziness and
fatigue. Data was presented at the 68th Annual Meeting of the
American Epilepsy Society in Seattle,
Wash. (5-9 December 2014).1
"Improving the lives of people with epilepsy and addressing
unmet medical needs is a priority for UCB. In our latest study,
brivaracetam used as adjunctive therapy significantly
reduced partial-onset seizure frequency for many patients. Over 80%
of patients in this study had a history of taking two or more AEDs
and almost half had a history of taking five or more AEDs," said
Professor Dr. Iris Loew-Friedrich,
Chief Medical Officer and Executive Vice President UCB. "We
are now focused on the next important step for brivaracetam with
applications to US and EU regulatory authorities planned for early
2015."
"This first presentation of primary study results from the
latest Phase 3 brivaracetam study is anticipated by the
epilepsy community. The two primary outcomes in this study
evaluating adjunctive brivaracetam in the treatment of
partial-onset seizures in adults with epilepsy were statistically
significant and clinically relevant," said Dr. Pavel Klein, Director, Mid-Atlantic Epilepsy and
Sleep Center, Bethesda, MD.
Efficacy results1
- Both brivaracetam doses (100 and 200
mg/day) demonstrated statistically significant percent reductions
in partial-onset seizure frequency per 28 days over placebo (22.8%
[n=252] and 23.2% [n=249] for 100 and 200 mg/day, respectively,
p<0.001)
- The 50% responder rate for brivaracetam 100 and 200 mg/day were 38.9% (98/252) and
37.8% (94/249), compared with 21.6% (56/259) for placebo,
p<0.001 for both dose arms. The odds ratios vs. placebo were
2.39 (95% Confidence Interval: 1.6,3.6) and 2.19 (95% Confidence
Interval:1.5,3.3) for brivaracetam 100 and
200 mg/day, respectively
Safety results1
- Treatment-emergent adverse events occurred in 68.4% (173/253)
and 66.8% (167/250) of patients in the brivaracetam 100 and 200 mg/day groups, respectively, and
in 59.4% (155/261) of patients in the placebo group
- The most commonly reported adverse events (greater than or
equal to 5%) for the combined brivaracetam
groups (n=503) and the placebo group (n=261) were somnolence (18.1%
vs. 7.7%), dizziness (12.3% vs. 5.0%), fatigue (9.5% vs. 3.8%) and
headache (7.4% vs. 8.4%)
- Study-discontinuation rates (for any reason) were 11.4% and
10.4 % for brivaracetam 100 and 200
mg/day, respectively, vs. 6.5% for placebo
About the Phase 3 study1
This Phase 3, multicentre, randomized, double-blind,
placebo-controlled study enrolled adults (greater than or equal to
16-80 years) with refractory partial-onset seizures whether or not
secondary generalized, and not fully controlled despite treatment
with one or two concomitant AEDs. In the study, 768 epilepsy
patients with partial-onset seizures, were randomized (1:1:1) to
adjunctive brivaracetam (100 or 200 mg/day) or placebo for a
12-week Treatment Period after having completed an 8-week
prospective Baseline Period. Patients taking levetiracetam,
either as concomitant antiepileptic drug or within 90 days prior to
Visit 1 were excluded. The primary efficacy outcome in the US was
the percent reduction over placebo in 28-day adjusted partial-onset
seizure frequency. The primary endpoint in the EU was the 50%
responder rate based on percent reduction in partial-onset seizure
frequency from Baseline to end of the Treatment Period.
NOTES TO EDITORS
About brivaracetam and the clinical development
program
Discovered and developed by UCB, brivaracetam is a
selective synaptic vesicle protein 2A ligand.2,3 The
phase 3 clinical development plan for
brivaracetam consisted of the following
studies:
N01252: an evaluation of the efficacy and
safety/tolerability of adjunctive brivaracetam 20, 50, and
100 mg/day compared with placebo over 12 weeks, in 399 randomized
patients (greater than or equal to 16 to 70 years) with
partial-onset seizures not fully controlled despite treatment with
1-2 concomitant AEDs.4
N01253: an evaluation of the efficacy and
safety/tolerability of adjunctive brivaracetam at doses of
5, 20, and 50 mg/day compared with placebo over 12 weeks, in 400
randomized patients (greater than or equal to 16 to 70 years) with
partial-onset seizures, not fully controlled despite treatment with
1-2 concomitant AEDs.5
N01254: an evaluation of the safety and tolerability of
adjunctive brivaracetam given at individualized tailored
doses between 20 and 150 mg/day, compared with placebo over 16
weeks, in 480 randomized patients (greater than or equal to 16 to
70 years) with uncontrolled epilepsy (up to 20% could be patients
with generalized epilepsy), not fully controlled despite treatment
with 1-3 concomitant AEDs.6
N01358: an evaluation of the efficacy and safety of
adjunctive brivaracetam 100 and 200 mg/day compared with
placebo over 12 weeks in 768 randomized patients (greater than or
equal to 16 to 80 years) with partial-onset seizures, not fully
controlled despite treatment with 1-2 concomitant
AEDs.1
About Epilepsy7-9
Epilepsy is a chronic neurological disorder affecting
approximately 65 million people worldwide and more than 2 million
people in the US. It is the fourth most common neurological
disorder in the US. Although epilepsy may be linked to
factors such as health conditions, race and age, it can develop in
anyone at any age. In the US, approximately 1 in 26 people will
develop epilepsy in their lifetime.
It is considered to be a disease of the brain defined by any of
the following conditions: (1) at least two unprovoked (or reflex)
seizures occurring >24 hours apart; (2) one unprovoked (or
reflex) seizure and a probability of further seizures similar to
the general recurrence risk (at least 60%) after two unprovoked
seizures, occurring over the next 10 years; (3) diagnosis of an
epilepsy syndrome.
About UCB in Epilepsy
UCB has a rich heritage in epilepsy with over 20 years of
experience in the research and development of antiepileptic drugs.
As a company with a long-term commitment to epilepsy research our
goal is to address unmet medical needs. Our scientists are proud to
contribute to advances in the understanding of epilepsy and its
treatment. We partner and create super-networks with world-leading
scientists and clinicians in academic institutions, pharmaceutical
companies and other organizations who share our goals. At UCB, we
are inspired by patients and driven by science in our commitment to
support patients with epilepsy.
For further information
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Antje
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Eimear
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Global
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Investor Relations,
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Brand Communications,
UCB
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T +32 2 559 92
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france.nivelle@ucb.com
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antje.witte@ucb.com
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eimear.obrien@ucb.com
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References
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1.
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Klein P., et
al. A Randomized, Double-blind, Placebo-controlled,
Multicenter, Parallel-group Study to Evaluate the Efficacy and
Safety of Brivaracetam in Adult Patients with Partial Onset
Seizures. Presented at AES 2014
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2.
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Kenda, B.M., et
al., Discovery of 4-Substituted Pyrrolidone Butanamides as New
Agents with Significant Antiepileptic Activity. Journal of
Medicinal Chemistry, 2004. 47(3): 530-549.
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3.
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Gillard, M., et
al., Binding characteristics of brivaracetam, a selective, high
affinity SV2A ligand in rat, mouse and human brain: relationship to
anti-convulsant properties. Eur J Pharmacol, 2011. 664(1-3):
36-44
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4.
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Ryvlin, P., et
al., Adjunctive brivaracetam in adults with uncontrolled focal
epilepsy: results from a double-blind, randomized,
placebo-controlled trial. Epilepsia, 2014. 55(1):47-56
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5.
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Biton, V., et
al., Brivaracetam as adjunctive treatment for uncontrolled
partial epilepsy in adults: a phase III randomized, double-blind,
placebo-controlled trial. Epilepsia, 2014. 55(1): 57-66
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6.
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Kwan, P., et
al., Adjunctive brivaracetam for uncontrolled focal and
generalized epilepsies: results of a phase III, double-blind,
randomized, placebo-controlled, flexible-dose trial. Epilepsia,
2014. 55(1):38-46
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7.
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Fisher, R.S., et
al., ILAE Official Report: A practical clinical definition of
epilepsy. Epilepsia, 2014. 55(4): 475-482
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8.
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Institute of
Medicine. Epilepsy Across the Spectrum. Promoting Health and
Understanding, Washington, DC: The National Academic Press, 2012
brief report. Accessed 29th October 2014 from
http://www.iom.edu/~/media/Files/Report%20Files/2012/Epilepsy/epilepsy_rb.pdf
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9.
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The Epilepsy
Foundation of America. Who gets epilepsy? Accessed 29th October
2014 from http://www.epilepsy.com/learn/epilepsy-101/who-gets-epilepsy
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About UCB
UCB, Brussels,
Belgium (www.ucb.com) is a global biopharmaceutical company
focused on the discovery and development of innovative medicines
and solutions to transform the lives of people living with severe
diseases of the immune system or of the central nervous system.
With more than 8500 people in approximately 40 countries, the
company generated revenue of € 3.4 billion in 2013. UCB is listed
on Euronext Brussels (symbol: UCB). Follow us on Twitter:
@UCB_news
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