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青春期后正向调节α5GABAA 受体以性别特异性方式改善丙戊酸致产前大鼠自闭症样特征。

Postweaning positive modulation of α5GABAA receptors improves autism-like features in prenatal valproate rat model in a sex-specific manner.

机构信息

Department of Pharmacology, University of Belgrade - Faculty of Pharmacy, Belgrade, Serbia.

Centre for Laser Microscopy, Institute of Physiology and Biochemistry "Jean Giaja", University of Belgrade - Faculty of Biology, Belgrade, Serbia.

出版信息

Autism Res. 2022 May;15(5):806-820. doi: 10.1002/aur.2699. Epub 2022 Mar 10.

Abstract

Autism spectrum disorder (ASD), as a common neurodevelopmental disorder that encompasses impairments in social communication and interaction, as well as repetitive and restrictive behavior, still awaits an effective treatment strategy. The involvement of GABAergic neurotransmission, and especially a deficit of GABA receptors that contain the α5 subunits, were implicated in pathogenesis of ASD. Therefore, we tested MP-III-022, a positive allosteric modulator (PAM) selective for α5GABAA receptors, in Wistar rats prenatally exposed to valproic acid, as an animal model useful for studying ASD. Postweaning rats of both sexes were treated for 7 days with vehicle or MP-III-022 at two doses pharmacokinetically determined as selective, and thereafter tested in a behavioral battery (social interaction test, elevated plus maze, spontaneous locomotor activity, and standard and reverse Morris water maze). Additional rats were used for establishing a primary neuronal culture and performing calcium imaging, and determination of hippocampal mRNA levels of GABRA5, NKCC1, and KCC2. MP-III-022 prevented impairments in many parameters connected with social, repetitive and restrictive behavioral domains. The lower and higher dose was more effective in males and females, respectively. Intriguingly, MP-III-022 elicited certain changes in control animals similar to those manifested in valproate animals themselves. Behavioral results were mirrored in GABA switch and spontaneous neuronal activity, assessed with calcium imaging, and also in expression changes of three genes analyzed. Our data support a role of α5GABAA receptors in pathophysiology of ASD, and suggest a potential application of selective PAMs in its treatment, that needs to be researched in a sex-specific manner. LAY SUMMARY: In rats prenatally exposed to valproate as a model of autism, a modulator of α5GABAA receptors ameliorated social, repetitive and restrictive impairments, and, intriguingly, elicited certain autism-like changes in control rats. Behavioral results were mirrored in GABA switch and spontaneous neuronal activity, and partly in gene expression changes. This shows a role of α5GABAA receptors in pathophysiology of ASD, and a potential application of their selective modulators in its treatment.

摘要

自闭症谱系障碍(ASD)是一种常见的神经发育障碍,包括社交沟通和互动障碍以及重复和受限的行为。目前仍缺乏有效的治疗策略。GABA 能神经传递的参与,特别是包含α5 亚单位的 GABA 受体的缺失,与 ASD 的发病机制有关。因此,我们在产前接触丙戊酸的 Wistar 大鼠中测试了 MP-III-022,这是一种对α5GABAA 受体具有正变构调节作用(PAM)的化合物,作为研究 ASD 的有用动物模型。两性幼鼠在断奶后用载体或两种剂量的 MP-III-022 治疗 7 天,这两种剂量根据药代动力学确定为选择性的,然后在行为测试中进行测试(社交互动测试、高架十字迷宫、自发运动活动以及标准和反向 Morris 水迷宫)。额外的大鼠用于建立原代神经元培养物并进行钙成像,并测定海马 GABRA5、NKCC1 和 KCC2 的 mRNA 水平。MP-III-022 可预防与社交、重复和限制性行为领域相关的许多参数的损伤。较低和较高剂量在雄性和雌性中分别更有效。有趣的是,MP-III-022 在对照动物中引起了某些类似于丙戊酸动物自身表现出的变化。行为结果与钙成像评估的 GABA 转换和自发神经元活动以及分析的三个基因的表达变化相吻合。我们的数据支持α5GABAA 受体在 ASD 病理生理学中的作用,并表明选择性 PAMs 在其治疗中的潜在应用,这需要以性别特异性的方式进行研究。

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