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Network Analysis of Genome-Wide Selective Constraint Reveals a Gene Network Active in Early Fetal Brain Intolerant of Mutation

机译:全基因组选择性约束的网络分析揭示了在早期胎儿脑不耐受突变中活跃的基因网络。

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摘要

Using robust, integrated analysis of multiple genomic datasets, we show that genes depleted for non-synonymous de novo mutations form a subnetwork of 72 members under strong selective constraint. We further show this subnetwork is preferentially expressed in the early development of the human hippocampus and is enriched for genes mutated in neurological Mendelian disorders. We thus conclude that carefully orchestrated developmental processes are under strong constraint in early brain development, and perturbations caused by mutation have adverse outcomes subject to strong purifying selection. Our findings demonstrate that selective forces can act on groups of genes involved in the same process, supporting the notion that purifying selection can act coordinately on multiple genes. Our approach provides a statistically robust, interpretable way to identify the tissues and developmental times where groups of disease genes are active.
机译:使用多个基因组数据集的可靠,综合的分析,我们显示,由于非同义的从头突变而耗竭的基因在强大的选择约束下形成了由72个成员组成的子网络。我们进一步表明,该子网络优先在人类海马的早期发育中表达,并丰富了神经系统孟德尔疾病中突变的基因。因此,我们得出的结论是,精心策划的发育过程在早期大脑发育中受到强大的约束,并且由突变引起的摄动具有不利的结果,这取决于强大的纯化选择。我们的发现表明,选择性力可以作用于同一过程中涉及的基因组,从而支持纯化选择可以协同作用于多个基因的观点。我们的方法提供了一种统计上可靠的,可解释的方式来识别疾病基因组活跃的组织和发育时期。

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