A phase II/III trial of bitopertin monotherapy compared with placebo in patients with an acute exacerbation of schizophrenia – Results from the CandleLyte study

Abstract Bitopertin is a glycine reuptake inhibitor postulated to improve N-methyl- d -aspartate receptor hypofunction by increasing synaptic glycine concentrations. This randomised, double-blind, placebo- and active-controlled phase II/III trial evaluated the efficacy and safety of bitopertin monot...

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Bibliographic Details
Published in:European neuropsychopharmacology 2014-07, Vol.24 (7), p.1024-1036
Main Authors: Bugarski-Kirola, D, Wang, A, Abi-Saab, D, Blättler, T
Format: Article
Language:English
Subjects:
Acute exacerbation
Adult
Antipsychotic Agents - therapeutic use
Benzodiazepines - therapeutic use
Bitopertin
Double-Blind Method
Female
Glycine reuptake inhibitor
Humans
Internal Medicine
Male
Middle Aged
Monotherapy
NMDA receptor
Piperazines - therapeutic use
Psychiatry
Schizophrenia
Schizophrenia - drug therapy
Sulfones - therapeutic use
Treatment Outcome
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Summary:Abstract Bitopertin is a glycine reuptake inhibitor postulated to improve N-methyl- d -aspartate receptor hypofunction by increasing synaptic glycine concentrations. This randomised, double-blind, placebo- and active-controlled phase II/III trial evaluated the efficacy and safety of bitopertin monotherapy over 4 weeks in patients with acute exacerbation of schizophrenia. Of 301 patients randomised, 299 received placebo ( n =80), bitopertin 10 mg ( n =80) or 30 mg ( n =77), or olanzapine 15 mg ( n= 62). The primary endpoint, change from baseline in mean Positive and Negative Syndrome Scale (PANSS) total score, showed non-statistically significant improvements with bitopertin 30 mg and olanzapine vs. placebo: bitopertin 10 mg (–11.7; standard error [SE], 1.89; p =0.945), bitopertin 30 mg (–15.3; SE, 1.87; p =0.211), olanzapine (–14.9; SE, 2.13; p =0.295) and placebo (–11.9; SE, 1.90). The PANSS positive subscale score, a secondary endpoint, also showed improvement with bitopertin 30 mg ( p =0.030) whereas a trend was observed with olanzapine ( p =0.072) vs. placebo. Although not statistically significant, bitopertin 30 mg and olanzapine reduced overall illness severity (Clinical Global Impression–Severity Scale; p =0.098 and p =0.126, respectively). More patients receiving bitopertin 30 mg (51.3%) or olanzapine (52.5%) than placebo (32.9%) were ready for hospital discharge at Week 4 (bitopertin, p =0.014; olanzapine, p =0.024). In summary, this study failed due to lack of statistical separation of either bitopertin or olanzapine (active control) from placebo on the primary endpoint. Of interest, improved positive symptoms and readiness for hospital discharge were associated with both bitopertin and olanzapine treatment. Bitopertin was safe and well tolerated in this study.
ISSN:0924-977X
1873-7862
DOI:10.1016/j.euroneuro.2014.03.007