自闭症患者精神疾病家族发病率与新生基因突变之间的关系。

Autism Research and Treatment Pub Date : 2017-01-01 Epub Date: 2017-11-08 DOI:10.1155/2017/9371964
Kyleen Luhrs, Tracey Ward, Caitlin M Hudac, Jennifer Gerdts, Holly A F Stessman, Evan E Eichler, Raphael A Bernier
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引用次数: 5

摘要

本研究的目的是检查遗传和家族风险因素在自闭症谱系障碍(ASD)儿童中具有不同的新生遗传事件的合流。我们假设,相对于结构突变,基因破坏突变与家族性精神疾病的发生率降低有关。参与者包括四组自闭症儿童家庭:新生的重复拷贝数变异(DUP, n = 62)、新生的缺失拷贝数变异(DEL, n = 74)、新生的可能基因破坏突变(LGDM, n = 267)和没有已知遗传病因的儿童(NON, n = 2111)。精神疾病的家族发病率是通过半结构化访谈计算出来的。结果表明,与DEL和LGDM家族相比,DUP家族的精神疾病总体发生率增加,这与父亲的精神病史有关,尤其是抑郁症。总体而言,与父亲的精神病史相比,LGDM家庭的母亲精神病史中抑郁症的发生率更高,而与DUP家庭相比,LGDM家庭的父亲精神病史中焦虑症的发生率更高。这些发现支持了遗传病因和家族因素与ASD风险相关的概念,并强调了针对这些关系继续开展工作的迫切需要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Associations between Familial Rates of Psychiatric Disorders and De Novo Genetic Mutations in Autism.

The purpose of this study was to examine the confluence of genetic and familial risk factors in children with Autism Spectrum Disorder (ASD) with distinct de novo genetic events. We hypothesized that gene-disrupting mutations would be associated with reduced rates of familial psychiatric disorders relative to structural mutations. Participants included families of children with ASD in four groups: de novo duplication copy number variations (DUP, n = 62), de novo deletion copy number variations (DEL, n = 74), de novo likely gene-disrupting mutations (LGDM, n = 267), and children without a known genetic etiology (NON, n = 2111). Familial rates of psychiatric disorders were calculated from semistructured interviews. Results indicated overall increased rates of psychiatric disorders in DUP families compared to DEL and LGDM families, specific to paternal psychiatric histories, and particularly evident for depressive disorders. Higher rates of depressive disorders in maternal psychiatric histories were observed overall compared to paternal histories and higher rates of anxiety disorders were observed in paternal histories for LGDM families compared to DUP families. These findings support the notion of an additive contribution of genetic etiology and familial factors are associated with ASD risk and highlight critical need for continued work targeting these relationships.

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发文量
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审稿时长
21 weeks
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