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Regulatory variations in the era of next-generation sequencing: Implications for clinical molecular diagnostics

机译:下一代测序时代的法规差异:对临床分子诊断的意义

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With the successful identification of many protein-coding genes, the focus has now shifted toward deciphering functions of non-protein-coding regions that direct spatiotemporal and quantitative aspects of protein expression. Recent advances in our understanding of the regulatory architecture of the human genome coincide with growing evidence that changes in regulatory sequences are associated with human disease. Several recent reviews have highlighted disease-causing potential of aberrations in transcriptional and splicing regulatory elements as well as non-protein-coding RNA. Although changes in regulatory sequences generally produce milder biological effects than their protein-coding counterparts, many act as independent risk factors for common complex disorders or as genetic modifiers for "primary" disease-causing loci. Here, we review bioinformatics and experimental approaches that are used to identify regulatory sequences and assess pathogenicity of regulatory changes. We describe the current state of knowledge on disease-causing changes in regulatory sequences, challenge protein-centric views, and discuss complexities and solutions pertaining to the interpretation of regulatory changes in the next-generation sequencing era.
机译:随着许多蛋白质编码基因的成功鉴定,现在的重点已转向解密非蛋白质编码区域的功能,这些区域指导蛋白质表达的时空和定量方面。我们对人类基因组调控结构的了解的最新进展与越来越多的证据表明调控序列的变化与人类疾病有关。最近的一些评论强调了转录和剪接调控元件以及非蛋白质编码RNA中引起畸变的致病潜力。尽管调节序列的变化通常会比编码蛋白的序列产生更温和的生物学效果,但许多变化可作为常见复杂疾病的独立危险因素或“主要”致病基因座的遗传修饰因子。在这里,我们审查了生物信息学和实验方法,这些方法可用于识别调节序列并评估调节变化的致病性。我们描述了有关致病性调控序列变化的知识的现状,挑战了以蛋白质为中心的观点,并讨论了与下一代测序时代中调控变化的解释有关的复杂性和解决方案。

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