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[一种无多巴胺受体阻断作用的抗精神病药物?]

[An antipsychotic without dopamine receptor blockade?].

作者信息

Spoelstra S K, Bruggeman R, Knegtering H

出版信息

Tijdschr Psychiatr. 2021;63(11):804-809.

Abstract

BACKGROUND

Current antipsychotic treatment is suboptimal. There is an urgent need for new antipsychotics with new mechanisms of action. SEP-363856 is a trace amine-associated receptor 1 (TAAR1) agonist and a serotonin 5-HT1a agonist with potential antipsychotic properties.

AIM

To describe the rationale for the development of SEP-363856, the pharmacology of TAAR1/5-HT1a agonists, and the clinical efficacy of SEP-363856.

METHOD

A narrative review of the literature using PubMed, Embase and PsychINFO.

RESULTS

Six publications were identified, one of which was a phase 2 clinical trial with SEP-363856. This phase 2 study shows that SEP-363856 is an effective and well-tolerated antipsychotic; positive, but also negative symptoms decreased; motor side effects (akathisia) and prolactin increase did not occur, while metabolic side effects hardly occurred. Reported side-effects were somnolence and nausea. The antipsychotic activity of SEP-363856 appears to be (pre)clinical not based on D2 antagonism, but on TAAR1 and 5-HT1a agonism.

CONCLUSION

TAAR1 and 5-HT1a agonists such as SEP-363856 may be a treatment option for psychosis. Hopefully they can be further developed into an antipsychotic with a favorable effectiveness and tolerability profile.

摘要

背景

目前的抗精神病药物治疗效果欠佳。迫切需要具有新作用机制的新型抗精神病药物。SEP-363856是一种与痕量胺相关受体1(TAAR1)激动剂以及5-羟色胺5-HT1a激动剂,具有潜在的抗精神病特性。

目的

阐述SEP-363856的研发原理、TAAR1/5-HT1a激动剂的药理学以及SEP-363856的临床疗效。

方法

使用PubMed、Embase和PsychINFO对文献进行叙述性综述。

结果

共检索到6篇文献,其中1篇为SEP-363856的2期临床试验。该2期研究表明,SEP-363856是一种有效且耐受性良好的抗精神病药物;阳性症状和阴性症状均有所减轻;未出现运动副作用(静坐不能)和催乳素升高的情况,代谢副作用也几乎未发生。报告的副作用为嗜睡和恶心。SEP-363856的抗精神病活性在临床前似乎并非基于D2拮抗作用,而是基于TAAR1和5-HT1a激动作用。

结论

SEP-363856等TAAR1和5-HT1a激动剂可能是治疗精神病的一种选择。有望将它们进一步开发成一种有效性和耐受性良好的抗精神病药物。

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