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Towards a molecular characterization of autism spectrum disorders: an exome sequencing and systems approach

机译:对自闭症谱系障碍的分子表征:外显子组测序和系统方法

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摘要

The hypothetical ‘AXAS' gene network model that profiles functional patterns of heterogeneous DNA variants overrepresented in autism spectrum disorder (ASD), X-linked intellectual disability, attention deficit and hyperactivity disorder and schizophrenia was used in this current study to analyze whole exome sequencing data from an Australian ASD cohort. An optimized DNA variant filtering pipeline was used to identify loss-of-function DNA variations. Inherited variants from parents with a broader autism phenotype and de novo variants were found to be significantly associated with ASD. Gene ontology analysis revealed that putative rare causal variants cluster in key neurobiological processes and are overrepresented in functions involving neuronal development, signal transduction and synapse development including the neurexin trans-synaptic complex. We also show how a complex gene network model can be used to fine map combinations of inherited and de novo variations in families with ASD that converge in the L1CAM pathway. Our results provide an important step forward in the molecular characterization of ASD with potential for developing a tool to analyze the pathogenesis of individual affected families.
机译:在当前的研究中,使用了假设的“ AXAS”基因网络模型,该模型描述了自闭症谱系障碍(ASD),X连锁智力残疾,注意力缺陷和活动过度障碍和精神分裂症中过分代表的异质DNA变体的功能模式,用于分析整个外显子组测序数据来自澳大利亚ASD队列。优化的DNA变体过滤管道用于识别功能丧失的DNA变体。发现具有更广泛的自闭症表型的父母的遗传变异和从头变异与ASD显着相关。基因本体分析表明,假定的罕见因果变异体聚集在关键的神经生物学过程中,并且在涉及神经元发育,信号转导和突触发育(包括神经毒素跨突触复合体)的功能中被过度表达。我们还展示了如何使用复杂的基因网络模型来细化图谱,这些图谱是在L1CAM途径中收敛的ASD家族中遗传和从头变异的组合。我们的结果为ASD的分子表征迈出了重要的一步,具有开发分析单个受影响家庭发病机制的潜力。

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