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VMAT2 抑制剂治疗迟发性运动障碍。

VMAT2 inhibitors for the treatment of tardive dyskinesia.

机构信息

Emory University Department of Neurology, Atlanta, GA, United States.

Emory University Department of Neurology, Atlanta, GA, United States.

出版信息

J Neurol Sci. 2018 Jun 15;389:43-47. doi: 10.1016/j.jns.2018.02.006. Epub 2018 Feb 5.

Abstract

Tardive dyskinesia (TD) is an often disabling hyperkinetic movement disorder caused by exposure to dopamine receptor blocking agents. Although initially thought to most commonly occur with typical antipsychotics, the incidence is likely similar with atypical antipsychotics and antiemetics such as metoclopramide. Increased prescribing of these agents as well as low rates of remission have contributed to a rising prevalence of TD. Although this condition was described nearly 60 years ago, it is only within the past year that two novel therapeutic agents were FDA approved. Characterization of the VMAT2 inhibitor tetrabenazine, which was identified as a therapeutic agent for TD in older clinical trials, has yielded two distinct pharmacologic strategies to optimize response. The first strategy, used to create deutetrabenazine, employed deuterization of tetrabenazine to stabilize the pharmacokinetics and eliminate high peak plasma levels. The second strategy was the creation of a prodrug, valbenazine, for the two most active isoforms of tetrabenazine that also resulted in more stable pharmacokinetics and eliminated peak plasma levels. Both agents have been demonstrated to be effective and safe for the treatment of TD in multicenter, controlled trials and their development has led to a resurgence of interest in the characterization and treatment of this movement disorder.

摘要

迟发性运动障碍(TD)是一种常导致运动障碍的障碍,由多巴胺受体阻断剂暴露引起。虽然最初认为它最常发生于典型的抗精神病药物,但非典型抗精神病药物和止吐药(如甲氧氯普胺)的发病率可能相似。这些药物的处方增加以及缓解率低导致 TD 的患病率上升。尽管这种情况在近 60 年前就已被描述,但直到过去一年,才批准了两种新型治疗药物。VMAT2 抑制剂替扎尼定的特性被确定为 older 临床试验中治疗 TD 的治疗药物,产生了两种优化反应的不同药理策略。第一种策略,用于制造氘代替扎尼定,采用氘代替扎尼定稳定其药代动力学并消除高血浆峰值水平。第二种策略是创建替扎贝嗪的前药,用于两种最活跃的替扎贝嗪同工酶,这也导致更稳定的药代动力学并消除了血浆峰值水平。在多中心对照试验中,这两种药物都被证明对 TD 的治疗有效且安全,其开发也重新激发了人们对这种运动障碍的特征和治疗的兴趣。

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