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Mining the 30UTR of Autism-implicated Genes for SNPs Perturbing MicroRNA Regulation

机译:挖掘自闭症相关基因的30UTR以干扰MicroRNA调控的SNP

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摘要

Autism spectrum disorder (ASD) refers to a group of childhood neurodevelopmental dis-orders with polygenic etiology. The expression of many genes implicated in ASD is tightly regulated by various factors including microRNAs (miRNAs), a class of noncoding RNAs 22 nucleotides in length that function to suppress translation by pairing with‘miRNA recognition elements’ (MREs) present in the 30untranslated region (30UTR) of target mRNAs. This emphasizes the role played by miRNAs in regulating neurogenesis, brain development and differentiation and hence any perturba-tions in this regulatory mechanism might affect these processes as well. Recently, single nucleotide polymorphisms (SNPs) present within 30UTRs of mRNAs have been shown to modulate existing MREs or even create new MREs. Therefore, we hypothesized that SNPs perturbing miRNA-medi-ated gene regulation might lead to aberrant expression of autism-implicated genes, thus resulting in disease predisposition or pathogenesis in at least a subpopulation of ASD individuals. We developed a systematic computational pipeline that integrates data from well-established databases. By following a stringent selection criterion, we identified 9 MRE-modulating SNPs and another 12 MRE-creating SNPs in the 30UTR of autism-implicated genes. These high-confidence candidate SNPs may play roles in ASD and hence would be valuable for further functional validation.
机译:自闭症谱系障碍(ASD)是指一组具有多基因病因的儿童神经发育障碍。与ASD有关的许多基因的表达受到各种因素的严格调控,包括microRNA(miRNA),这是一类长度为22个核苷酸的非编码RNA,其功能是与30个非翻译区中的“ miRNA识别元件”(MRE)配对,从而抑制翻译(30UTR)的目标mRNA。这强调了miRNA在调节神经发生,大脑发育和分化中所起的作用,因此在这种调节机制中的任何干扰也会影响这些过程。最近,已经显示出存在于mRNA的30UTR中的单核苷酸多态性(SNP)可以调节现有的MRE甚至产生新的MRE。因此,我们假设扰动miRNA介导的基因调控的SNP可能导致自闭症相关基因的异常表达,从而至少在ASD个体中导致疾病易感性或发病机理。我们开发了系统的计算管道,该管道整合了来自完善数据库的数据。通过遵循严格的选择标准,我们在自闭症相关基因的30UTR中鉴定了9个MRE调节SNP和另外12个MRE产生SNP。这些高可信度的候选SNP可能在ASD中发挥作用,因此对于进一步的功能验证很有用。

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    Department of Genetics, Dr. ALM PG Institute of Basic Medical Sciences, University of Madras, Taramani Campus, Chennai 600113, India;

    Department of Genetics, Dr. ALM PG Institute of Basic Medical Sciences, University of Madras, Taramani Campus, Chennai 600113, India;

    Department of Genetics, Dr. ALM PG Institute of Basic Medical Sciences, University of Madras, Taramani Campus, Chennai 600113, India;

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