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卡立氨酯(RWJ - 333369)。

Carisbamate (RWJ-333369).

作者信息

Novak Gerald P, Kelley Michael, Zannikos Peter, Klein Brian

机构信息

Johnson & Johnson, Pharmaceutical Research & Development L.L.C., Titusville, New Jersey 08560, USA.

出版信息

Neurotherapeutics. 2007 Jan;4(1):106-9. doi: 10.1016/j.nurt.2006.11.016.

Abstract

Carisbamate (RWJ-333369) is a novel neuromodulator, initially developed by SK Biopharmaceuticals (Fairlawn, NJ), under development by Johnson & Johnson Pharmaceutical Research and Development (La Jolla, CA). Carisbamate displays high potency in a broad range of rodent seizure models at doses well below those that produce CNS toxicity. Its mechanism of action has not been elucidated. Acute and chronic nonclinical toxicological studies have not revealed any significant abnormalities other than dose-related CNS toxicity. It is extensively metabolized, chiefly through glucuronidation and oxidation of the aliphatic side chain. There is little evidence of CYP metabolism. It has linear pharmacokinetics. Its clearance is increased by carbamazepine and to a lesser degree by oral contraceptives. Carisbamate slightly increases the clearance of valproic acid and lamotrigine. The most common adverse events in humans are headaches, dizziness, and somnolence, generally mild to moderate, occurring at doses of 1000 mg/day or more. A recently completed phase 2 study for adjunctive use in partial onset seizures showed efficacy at a dose that was well tolerated.

摘要

卡立普多(RWJ - 333369)是一种新型神经调节剂,最初由SK生物制药公司(新泽西州费尔劳恩)研发,现由强生制药研发公司(加利福尼亚州拉霍亚)进行后续开发。卡立普多在多种啮齿动物癫痫模型中,以远低于产生中枢神经系统毒性的剂量显示出高效能。其作用机制尚未阐明。急性和慢性非临床毒理学研究未发现除剂量相关的中枢神经系统毒性外的任何显著异常。它主要通过脂肪族侧链的葡萄糖醛酸化和氧化进行广泛代谢。几乎没有细胞色素P450(CYP)代谢的证据。它具有线性药代动力学。卡马西平可增加其清除率,口服避孕药在较小程度上也可增加其清除率。卡立普多会轻微增加丙戊酸和拉莫三嗪的清除率。在人类中最常见的不良事件是头痛、头晕和嗜睡,通常为轻至中度,发生在每日剂量1000毫克或更高时。最近完成的一项用于辅助治疗部分性发作的2期研究表明,在一个耐受性良好的剂量下具有疗效。

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Carisbamate (RWJ-333369).卡立氨酯(RWJ - 333369)。
Neurotherapeutics. 2007 Jan;4(1):106-9. doi: 10.1016/j.nurt.2006.11.016.
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