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利培酮的D2多巴胺受体占有率及其与锥体外系症状的关系:一项正电子发射断层扫描(PET)研究。

The D2 dopamine receptor occupancy of risperidone and its relationship to extrapyramidal symptoms: a PET study.

作者信息

Kapur S, Remington G, Zipursky R B, Wilson A A, Houle S

机构信息

Schizophrenia Research Program, Clarke Institute of Psychiatry, University of Toronto, ON, Canada.

出版信息

Life Sci. 1995;57(10):PL103-7. doi: 10.1016/0024-3205(95)02037-j.

Abstract

Risperidone is a recently introduced neuroleptic distinguished by a decreased incidence of extrapyramidal side effects (EPS). The mechanism of its low EPS is unclear. Since it has been shown that EPS is related to the level of D2 receptor occupancy, we studied nine patients receiving 2-6 mg/day of risperidone using [11C]-raclopride PET scans in order to determine the in vivo D2 receptor binding characteristics of risperidone. The mean level of receptor occupancy was 66% at 2 mg; 73% at 4 mg; and 79% at 6 mg. Three patients, those with the highest receptor occupancies, exhibited mild EPS, though none required anitparkinsonian medications. Our results suggest that at doses of 4-6 mg the in vivo D2 receptor occupancy of risperidone is similar to that of typical neuroleptics and higher than that of clozapine. This would suggest that the EPS benefits of risperidone cannot be explained by a low D2 binding but may be related to its high 5-HT2 affinity. However, the emergence of EPS at higher levels of D2 receptor occupancy, in this study and in previous clinical trials, would suggest that risperidone's high 5-HT2 affinity provides only a relative protection from EPS. And once the D2 occupancy exceeds a certain threshold this 'relative' 5-HT2-mediated protection from EPS may be lost.

摘要

利培酮是一种最近引入的抗精神病药物,其特点是锥体外系副作用(EPS)的发生率较低。其低EPS的机制尚不清楚。由于已经表明EPS与D2受体占有率水平有关,我们对9名每天接受2 - 6毫克利培酮治疗的患者进行了[11C] - 雷氯必利PET扫描,以确定利培酮在体内的D2受体结合特性。受体占有率的平均水平在2毫克时为66%;4毫克时为73%;6毫克时为79%。三名受体占有率最高的患者出现了轻度EPS,不过没有人需要使用抗帕金森药物。我们的结果表明,在4 - 6毫克的剂量下,利培酮在体内的D2受体占有率与典型抗精神病药物相似,且高于氯氮平。这表明利培酮EPS方面的优势不能用低D2结合来解释,而可能与其高5 - HT2亲和力有关。然而,在本研究和之前的临床试验中,在较高水平的D2受体占有率时出现了EPS,这表明利培酮的高5 - HT2亲和力仅提供了对EPS的相对保护。一旦D2占有率超过某个阈值,这种由5 - HT2介导的对EPS的“相对”保护可能会丧失。

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