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Revisiting Mendelian disorders through exome sequencing.

机译:通过外显子组测序重新探讨孟德尔疾病。

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Over the past several years, more focus has been placed on dissecting the genetic basis of complex diseases and traits through genome-wide association studies. In contrast, Mendelian disorders have received little attention mainly due to the lack of newer and more powerful methods to study these disorders. Linkage studies have previously been the main tool to elucidate the genetics of Mendelian disorders; however, extremely rare disorders or sporadic cases caused by de novo variants are not amendable to this study design. Exome sequencing has now become technically feasible and more cost-effective due to the recent advances in high-throughput sequence capture methods and next-generation sequencing technologies which have offered new opportunities for Mendelian disorder research. Exome sequencing has been swiftly applied to the discovery of new causal variants and candidate genes for a number of Mendelian disorders such as Kabuki syndrome, Miller syndrome and Fowler syndrome. In addition, de novo variants were also identified for sporadic cases, which would have not been possible without exome sequencing. Although exome sequencing has been proven to be a promising approach to study Mendelian disorders, several shortcomings of this method must be noted, such as the inability to capture regulatory or evolutionary conserved sequences in non-coding regions and the incomplete capturing of all exons.
机译:在过去的几年中,通过全基因组关联研究,更加关注解剖复杂疾病和性状的遗传基础。相反,孟德尔疾病很少受到关注,这主要是由于缺乏研究这些疾病的更新且更有效的方法。连锁研究以前一直是阐明孟德尔疾病遗传学的主要工具。但是,由新变异引起的极为罕见的疾病或零星病例不适用于本研究设计。由于高通量序列捕获方法和下一代测序技术的最新进展,外显子组测序现已在技术上变得可行且更具成本效益,这为孟德尔疾病研究提供了新的机会。外显子组测序已迅速应用于发现许多孟德尔疾病(例如歌舞uki综合症,米勒综合症和福勒综合症)的新因果变体和候选基因。此外,还鉴定了散发病例的从头变异,如果没有外显子组测序,这是不可能的。尽管外显子组测序已被证明是研究孟德尔疾病的一种有前途的方法,但必须指出该方法的一些缺点,例如无法在非编码区捕获调控或进化保守序列,以及所有外显子的捕获不完全。

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