在患有反社会人格障碍的极端冲动暴力男性中,受限基因、大脑特异基因和突触基因中的罕见蛋白质截断变体的负担加重。

IF 2.4 4区 心理学 Q2 BEHAVIORAL SCIENCES
Dita Mušálková, Anna Přistoupilová, Ivana Jedličková, Hana Hartmannová, Helena Trešlová, Lenka Nosková, Kateřina Hodaňová, Petra Bittmanová, Viktor Stránecký, Václav Jiřička, Michaela Langmajerová, Marc Woodbury-Smith, Mehdi Zarrei, Brett Trost, Stephen W. Scherer, Anthony J. Bleyer, Jan Vevera, Stanislav Kmoch
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引用次数: 0

摘要

人们对极端冲动暴力的遗传相关性知之甚少,而且很少有研究从临床和遗传学两方面描述了一大批受影响的个体。我们对 290 名患有反社会型人格障碍(APD)的男性患者进行了全外显子组测序(WES),分析了罕见蛋白质截断变体(rPTV)的谱系。结果与 314 名男性对照组和公开的基因型数据进行了比较。使用功能注释工具进行生物学解释。在不耐受功能缺失变异的基因中,参与者携带 rPTV 的几率明显更高(几率比 [OR] 2.06;p
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Increased burden of rare protein-truncating variants in constrained, brain-specific and synaptic genes in extremely impulsively violent males with antisocial personality disorder

Increased burden of rare protein-truncating variants in constrained, brain-specific and synaptic genes in extremely impulsively violent males with antisocial personality disorder

The genetic correlates of extreme impulsive violence are poorly understood, and there have been few studies that have characterized a large group of affected individuals both clinically and genetically. We performed whole exome sequencing (WES) in 290 males with the life-course-persistent, extremely impulsively violent form of antisocial personality disorder (APD) and analyzed the spectrum of rare protein-truncating variants (rPTVs). Comparisons were made with 314 male controls and publicly available genotype data. Functional annotation tools were used for biological interpretation. Participants were significantly more likely to harbor rPTVs in genes that are intolerant to loss-of-function variants (odds ratio [OR] 2.06; p < 0.001), specifically expressed in brain (OR 2.80; p = 0.036) and enriched for those involved in neurotransmitter transport and synaptic processes. In 60 individuals (20%), we identified rPTVs that we classified as clinically relevant based on their clinical associations, biological function and gene expression patterns. Of these, 37 individuals harbored rPTVs in 23 genes that are associated with a monogenic neurological disorder, and 23 individuals harbored rPTVs in 20 genes reportedly intolerant to loss-of-function variants. The analysis presents evidence in support of a model where presence of either one or several private, functionally relevant mutations contribute significantly to individual risk of life-course-persistent APD and reveals multiple individuals who could be affected by clinically unrecognized neuropsychiatric Mendelian disease. Thus, Mendelian diseases and increased rPTV burden may represent important factors for the development of extremely impulsive violent life-course-persistent forms of APD irrespective of their clinical presentation.

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来源期刊
Genes Brain and Behavior
Genes Brain and Behavior 医学-行为科学
CiteScore
6.80
自引率
4.00%
发文量
62
审稿时长
4-8 weeks
期刊介绍: Genes, Brain and Behavior was launched in 2002 with the aim of publishing top quality research in behavioral and neural genetics in their broadest sense. The emphasis is on the analysis of the behavioral and neural phenotypes under consideration, the unifying theme being the genetic approach as a tool to increase our understanding of these phenotypes. Genes Brain and Behavior is pleased to offer the following features: 8 issues per year online submissions with first editorial decisions within 3-4 weeks and fast publication at Wiley-Blackwells High visibility through its coverage by PubMed/Medline, Current Contents and other major abstracting and indexing services Inclusion in the Wiley-Blackwell consortial license, extending readership to thousands of international libraries and institutions A large and varied editorial board comprising of international specialists.
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