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马西替坦对视知觉注意力和瞳孔反应的影响在脆性 X 综合征患者观看面部照片时的表现。

Effects of mavoglurant on visual attention and pupil reactivity while viewing photographs of faces in Fragile X Syndrome.

机构信息

MIND Institute, University of California Davis Medical Center, Sacramento, California, United States of America.

Department of Psychiatry and Behavioral Sciences, University of California Davis School of Medicine, Sacramento, California, United States of America.

出版信息

PLoS One. 2019 Jan 17;14(1):e0209984. doi: 10.1371/journal.pone.0209984. eCollection 2019.

Abstract

BACKGROUND

Numerous preclinical studies have supported the theory that enhanced activation of mGluR5 signaling, due to the absence or reduction of the FMR1 protein, contributes to cognitive and behavioral deficits in patients with fragile X syndrome (FXS). However multiple phase 2 controlled trials in patients with FXS have failed to demonstrate efficacy of compounds that negatively modulate mGluR5, including two phase 2b randomized controlled trials (RCT) of mavoglurant (AFQ056, Novartis Pharma AG), when the primary measures of interest were behavioral ratings. This has cast some doubt onto the translation of the mGluR5 theory from animal models to humans with the disorder.

METHODS

We evaluated social gaze behavior-a key phenotypic feature of the disorder-and sympathetic nervous system influence on pupil size using a previously-validated eye tracking paradigm as a biobehavioral probe, in 57 adolescent or adult patients with FXS at baseline and following three months of blinded treatment with one of three doses of mavoglurant or placebo, within the context of the AFQ056 RCTs.

RESULTS

Patients with FXS treated with mavoglurant demonstrated increased total absolute looking time and number of fixations to the eye region while viewing human faces relative to baseline, and compared to those treated with placebo. In addition, patients had greater pupil reactivity to faces relative to baseline following mavoglurant treatment compared to placebo.

DISCUSSION

The study shows that negative modulation of mGluR5 activity improves eye gaze behavior and alters sympathetically-driven reactivity to faces in patients with FXS, providing preliminary evidence of this drug's impact on behavior in humans with the disorder.

摘要

背景

大量的临床前研究支持这样一种理论,即由于 FMR1 蛋白的缺失或减少,mGluR5 信号的增强激活导致脆性 X 综合征(FXS)患者的认知和行为缺陷。然而,在 FXS 患者中进行的多项 2 期对照试验未能证明负性调节 mGluR5 的化合物的疗效,包括两种 mavoglurant(AFQ056,诺华制药公司)的 2b 期随机对照试验(RCT),当主要关注的测量指标是行为评分时。这使得人们对从动物模型到患有该疾病的人类的 mGluR5 理论的转化产生了一些怀疑。

方法

我们评估了社会注视行为-该疾病的一个关键表型特征-以及自主神经系统对瞳孔大小的影响,使用了以前验证过的眼动追踪范式作为生物行为探针,在基线时对 57 名青少年或成年 FXS 患者进行了评估,并在 AFQ056 RCT 中对三种剂量的 mavoglurant 或安慰剂进行了为期三个月的盲法治疗后进行了评估。

结果

与基线相比,接受 mavoglurant 治疗的 FXS 患者在观看人脸时,总绝对注视时间和注视眼部区域的注视次数增加,与接受安慰剂治疗的患者相比。此外,与安慰剂治疗相比,mavoglurant 治疗后患者对人脸的瞳孔反应性更高。

讨论

该研究表明,mGluR5 活性的负性调节可改善 FXS 患者的眼注视行为,并改变自主神经驱动对人脸的反应性,为该药物对该疾病患者行为的影响提供了初步证据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e10f/6336311/70cdd64ebbdb/pone.0209984.g001.jpg

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