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Methods for routine diagnosis of genomic rearrangements: multiplex PCR-based methods and future perspectives.

机译:常规诊断基因组重排的方法:基于多重PCR的方法和未来展望。

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Germline and somatic genomic rearrangement play a relevant role in the pathogenesis of genetic disorders, and their identification is a fundamental task in molecular diagnosis. However, screening for structural genomic abnormalities is often not included in routine mutational analyses and consequently the proportion of rearrangements playing a pathogenic role in several genetic disorders is likely to be underestimated. A wide range of molecular techniques for the detection of large genomic rearrangements has been developed: some methods have the power to screen the whole genome, others are designed to analyze one or few loci that are known to be involved in a specific disease; some may detect balanced rearrangements, while others only unbalanced rearrangements; some are suitable for detection of germline abnormalities, yet others also detect somatic abnormalities. This review provides a brief summary of principles, applications and limitations of the methods available for the screening of genomic rearrangements, focusing on multiplex PCR-based protocols that are currently employed in routine detection of extended germline genomic deletions or duplications. Future developments based on microarray platforms and high-throughput sequencing are also discussed.
机译:胚系和体细胞基因组重排在遗传疾病的发病机理中起着重要作用,而它们的鉴定是分子诊断的基本任务。但是,常规突变分析通常不包括对结构基因组异常的筛查,因此可能会低估在几种遗传疾病中起致病作用的重排比例。已经开发出了多种检测大基因组重排的分子技术:一些方法具有筛选整个基因组的能力,另一些方法则用于分析一个或几个已知与特定疾病有关的基因座。一些可能检测到平衡的重排,而另一些则仅检测到不平衡的重排;一些适合检测种系异常,而另一些也可以检测体细胞异常。这篇综述简要概述了可用于筛选基因组重排的方法的原理,应用和局限性,重点介绍了目前在常规检测扩展种系基因组缺失或重复中使用的基于多重PCR的方案。还讨论了基于微阵列平台和高通量测序的未来发展。

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