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人类新生突变的全基因组模式与特性

Genome-wide patterns and properties of de novo mutations in humans.

作者信息

Francioli Laurent C, Polak Paz P, Koren Amnon, Menelaou Androniki, Chun Sung, Renkens Ivo, van Duijn Cornelia M, Swertz Morris, Wijmenga Cisca, van Ommen Gertjan, Slagboom P Eline, Boomsma Dorret I, Ye Kai, Guryev Victor, Arndt Peter F, Kloosterman Wigard P, de Bakker Paul I W, Sunyaev Shamil R

机构信息

Department of Medical Genetics, Center for Molecular Medicine, University Medical Center Utrecht, Utrecht, The Netherlands.

Division of Genetics, Brigham and Women's Hospital, Harvard Medical School, Boston, MA, USA.

出版信息

Nat Genet. 2015 Jul;47(7):822-826. doi: 10.1038/ng.3292. Epub 2015 May 18.

Abstract

Mutations create variation in the population, fuel evolution and cause genetic diseases. Current knowledge about de novo mutations is incomplete and mostly indirect. Here we analyze 11,020 de novo mutations from the whole genomes of 250 families. We show that de novo mutations in the offspring of older fathers are not only more numerous but also occur more frequently in early-replicating, genic regions. Functional regions exhibit higher mutation rates due to CpG dinucleotides and show signatures of transcription-coupled repair, whereas mutation clusters with a unique signature point to a new mutational mechanism. Mutation and recombination rates independently associate with nucleotide diversity, and regional variation in human-chimpanzee divergence is only partly explained by heterogeneity in mutation rate. Finally, we provide a genome-wide mutation rate map for medical and population genetics applications. Our results provide new insights and refine long-standing hypotheses about human mutagenesis.

摘要

突变在种群中产生变异,推动进化并引发遗传疾病。目前关于新生突变的知识并不完整,且大多是间接的。在此,我们分析了来自250个家庭全基因组中的11020个新生突变。我们发现,年长父亲的后代中的新生突变不仅数量更多,而且在早期复制的基因区域出现得更频繁。由于CpG二核苷酸,功能区域呈现出更高的突变率,并显示出转录偶联修复的特征,而具有独特特征的突变簇则指向一种新的突变机制。突变率和重组率分别与核苷酸多样性相关,人类与黑猩猩分歧的区域差异仅部分由突变率的异质性所解释。最后,我们提供了一张全基因组突变率图谱,用于医学和群体遗传学应用。我们的结果为人类诱变作用提供了新的见解,并完善了长期以来的假说。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f772/4485564/37fcb388cdf2/nihms-679155-f0001.jpg

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