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Genes, mutations, and human inherited disease at the dawn of the age of personalized genomics.

机译:个性化基因组学时代的来临之际,基因,突变和人类遗传疾病。

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The number of reported germline mutations in human nuclear genes, either underlying or associated with inherited disease, has now exceeded 100,000 in more than 3,700 different genes. The availability of these data has both revolutionized the study of the morbid anatomy of the human genome and facilitated "personalized genomics." With approximately 300 new "inherited disease genes" (and approximately 10,000 new mutations) being identified annually, it is pertinent to ask how many "inherited disease genes" there are in the human genome, how many mutations reside within them, and where such lesions are likely to be located? To address these questions, it is necessary not only to reconsider how we define human genes but also to explore notions of gene essentiality from recent novel insights into genome structure and function and through complete genome sequence information derived from multiple individual human genomes. However, a change in focus toward screening functional genomic elements as opposed to genes sensu stricto will be required if we are to capitalize fully on recent technical and conceptual advances and identify new types of disease-associated mutation within noncoding regions remote from the genes whose function they disrupt.
机译:人类核基因中潜在或与遗传性疾病相关的种系突变的报道数量现已超过3,700种,超过了100,000种。这些数据的可利用性已经彻底改变了人类基因组病态解剖学的研究,并促进了“个性化基因组学”的发展。每年大约鉴定出300个新的“遗传病基因”(和大约10,000个新突变),因此有必要询问人类基因组中有多少个“遗传病基因”,其中存在多少突变以及这些病灶在何处可能位于?为了解决这些问题,不仅有必要重新考虑我们如何定义人类基因,而且还需要从对基因组结构和功能的最新新颖见解以及从多个人类基因组中获得的完整基因组序列信息中探索基因重要性的概念。但是,如果我们要充分利用最新的技术和概念进展,并在远离其功能基因的非编码区中鉴定与疾病相关的新型突变,那么就需要改变侧重于筛选功能基因组元件而不是严格的基因。他们破坏了。

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