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Identifying Essential Cell Types and Circuits in Autism Spectrum Disorders

机译:识别自闭症谱系障碍中的基本细胞类型和电路

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摘要

Autism spectrum disorder (ASD) is highly genetic in its etiology, with potentially hundreds of genes contributing to risk. Despite this heterogeneity, these disparate genetic lesions may result in the disruption of a limited number of key cell types or circuits –information which could be leveraged for the design of therapeutic interventions. While hypotheses for cellular disruptions can be identified by postmortem anatomical analysis and expression studies of ASD risk genes, testing these hypotheses requires the use of animal models. In this review, we explore the existing evidence supporting the contribution of different cell types to ASD, specifically focusing on rodent studies disrupting serotonergic, GABAergic, cerebellar and striatal cell types, with particular attention to studies of the sufficiency of specific cellular disruptions to generate ASD-related behavioral abnormalities. This evidence suggests multiple cellular routes can create features of the disorder, though it is currently unclear if these cell types converge on a final common circuit. We hope that in the future, systematic studies of cellular sufficiency and genetic interaction will help to classify patients into groups by type of cellular disruptions which suggest tractable therapeutic targets.
机译:自闭症谱系障碍(ASD)在病因上具有高度遗传性,可能有数百种基因会引发风险。尽管存在异质性,但这些不同的遗传损伤可能会导致有限数量的关键细胞类型或电路破裂,这些信息可用于设计治疗性干预措施。虽然可以通过事后解剖分析和ASD风险基因的表达研究来确定细胞破坏的假说,但要检验这些假说需要使用动物模型。在这篇综述中,我们探索了支持不同细胞类型对ASD贡献的现有证据,特别是专注于破坏血清素能,GABA能,小脑和纹状体细胞类型的啮齿动物研究,尤其是对特定细胞破坏产生ASD的充分性的研究的关注。相关的行为异常。尽管目前尚不清楚这些细胞类型是否会在最终的公用回路中汇合,但该证据表明多种细胞途径可形成该疾病的特征。我们希望在将来,对细胞充足性和遗传相互作用的系统研究将有助于根据细胞破裂类型将患者分为几类,从而提出易于治疗的目标。

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