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吗啉胍的研发及其治疗脆性X综合征的潜力。

Development of mavoglurant and its potential for the treatment of fragile X syndrome.

作者信息

Gomez-Mancilla Baltazar, Berry-Kravis Elizabeth, Hagerman Randi, von Raison Florian, Apostol George, Ufer Mike, Gasparini Fabrizio, Jacquemont Sébastien

机构信息

Novartis Institutes for BioMedical Research Basel, Forum 1 , Novartis Campus, CH-4056 Basel , Switzerland +41 61 324 0164 ; +41 61 324 8913 ;

出版信息

Expert Opin Investig Drugs. 2014 Jan;23(1):125-34. doi: 10.1517/13543784.2014.857400. Epub 2013 Nov 20.

DOI:10.1517/13543784.2014.857400
PMID:24251408
Abstract

INTRODUCTION

Fragile X syndrome (FXS) is the most common inherited cause of intellectual disability. With no curative treatment available, current therapeutic approaches are aimed at symptom management. FXS is caused by silencing the FMR1 gene, which encodes FMRP; as loss of FMRP leads to the development of symptoms associated with FXS.

AREAS COVERED

In this evaluation, the authors examine the role of the metabotropic glutamate receptor 5 (mGluR5) in the pathophysiology of FXS, and its suitability as a target for rescuing the disease state. Furthermore, the authors review the evidence from preclinical studies of pharmacological interventions targeting mGluR5 in FXS. Lastly, the authors assess the findings from clinical studies in FXS, in particular the use of the Aberrant Behavior Checklist-Community Edition (ABC-C) and the recently developed ABC-C for FXS scale, as clinical endpoints to assess disease modification in this patient population.

EXPERT OPINION

There is cautious optimism for the successful treatment of the core behavioral and cognitive symptoms of FXS based on preclinical data in animal models and early studies in humans. However, the association between mGluR5-heightened responsiveness and the clinical phenotype in humans remains to be demonstrated. Many questions regarding the optimal treatment and outcome measures of FXS remain unanswered.

摘要

引言

脆性X综合征(FXS)是智力残疾最常见的遗传性病因。由于尚无治愈性治疗方法,目前的治疗方法旨在控制症状。FXS是由FMR1基因沉默引起的,该基因编码FMRP;因为FMRP的缺失会导致与FXS相关症状的出现。

涵盖领域

在本评估中,作者研究了代谢型谷氨酸受体5(mGluR5)在FXS病理生理学中的作用,以及其作为挽救疾病状态靶点的适用性。此外,作者回顾了针对FXS中mGluR5的药理学干预临床前研究的证据。最后,作者评估了FXS临床研究的结果,特别是异常行为检查表社区版(ABC-C)和最近开发的FXS专用ABC-C量表的使用情况,作为评估该患者群体疾病改善情况的临床终点。

专家意见

基于动物模型的临床前数据和人类早期研究,对于成功治疗FXS的核心行为和认知症状存在谨慎的乐观态度。然而,mGluR5反应性增强与人类临床表型之间的关联仍有待证实。关于FXS最佳治疗方法和结局指标的许多问题仍未得到解答。

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