Dystrophin genetic variants and autism.

Maria Rita Passos-Bueno, Claudia Ismania Samogy Costa, Mayana Zatz
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Abstract

Loss-of-function variants in the dystrophin gene, a well-known cause of muscular dystrophies, have emerged as a mutational risk mechanism for autism spectrum disorder (ASD), which in turn is a highly prevalent (~ 1%) genetically heterogeneous neurodevelopmental disorder. Although the association of intellectual disability with the dystrophinopathies Duchenne (DMD) and Becker muscular dystrophy (BMD) has been long established, their association with ASD is more recent, and the dystrophin genotype-ASD phenotype correlation is unclear. We therefore present a review of the literature focused on the ASD prevalence among dystrophinopathies, the relevance of the dystrophin isoforms, and most particularly the relevance of the genetic background to the etiology of ASD in these patients. Four families with ASD-DMD/BMD patients are also reported here for the first time. These include a single ASD individual, ASD-discordant and ASD-concordant monozygotic twins, and non-identical ASD triplets. Notably, two unrelated individuals, which were first ascertained because of the ASD phenotype at ages 15 and 5 years respectively, present rare dystrophin variants still poorly characterized, suggesting that some dystrophin variants may compromise the brain more prominently. Whole exome sequencing in these ASD-DMD/BMD individuals together with the literature suggest, although based on preliminary data, a complex and heterogeneous genetic architecture underlying ASD in dystrophinopathies, that include rare variants of large and medium effect. The need for the establishment of a consortia for genomic investigation of ASD-DMD/BMD patients, which may shed light on the genetic architecture of ASD, is discussed.

Abstract Image

肌营养不良蛋白基因变异与自闭症
肌营养不良蛋白基因的功能缺失变异是肌肉营养不良的一个众所周知的原因,它已成为自闭症谱系障碍(ASD)的一种突变风险机制,而ASD又是一种高度流行的疾病(~ 1%)遗传异质性神经发育障碍。尽管智力残疾与杜氏肌营养不良症(DMD)和贝克尔肌营养不良(BMD)的相关性早已确立,但它们与ASD的相关性是最近才发现的,而且肌营养不良蛋白基因型与ASD表型的相关性尚不清楚。因此,我们对文献进行了综述,重点关注肌营养不良蛋白病中ASD的患病率、肌营养不良素亚型的相关性,尤其是遗传背景与这些患者ASD病因的相关性。本文还首次报道了四个ASD-DDMD/BMD患者家族。其中包括单个ASD个体、ASD不一致和ASD一致的单卵双胞胎以及非同卵ASD三胞胎。值得注意的是,两个无关的个体分别在15岁和5岁时因ASD表型而首次被确定,它们呈现出罕见的肌营养不良蛋白变体,但其特征仍然很差,这表明一些肌营养不良素变体可能会更显著地损害大脑。这些ASD-DDMD/BMD个体的全外显子组测序以及文献表明,尽管基于初步数据,但肌营养不良患者ASD的遗传结构复杂且异质,其中包括罕见的大中型变异。讨论了建立ASD-DDMD/BMD患者基因组研究联盟的必要性,这可能会揭示ASD的遗传结构。
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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CiteScore
1.90
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