Population sequencing data reveal a compendium of mutational processes in the human germ line

Vladimir B. Seplyarskiy(Brigham and Women's Hospital), Ruslan Soldatov(Harvard University), Evan Koch(Brigham and Women's Hospital), Ryan J. McGinty(Brigham and Women's Hospital), Jakob M. Goldmann(Radboud University Nijmegen), Ryan D. Hernandez(University of California, San Francisco), Kathleen C. Barnes(University of Colorado Denver), Adolfo Correa(Jackson Memorial Hospital), Esteban G. Burchard(University of California, San Francisco), Patrick T. Ellinor(Broad Institute), Stephen T. McGarvey(Brown University), Braxton D. Mitchell(University of Maryland, Baltimore), Ramachandran S. Vasan(Boston University), Susan Redline(Brigham and Women's Hospital), Edwin K. Silverman(Brigham and Women's Hospital), Scott T. Weiss(Brigham and Women's Hospital), Donna K. Arnett(University of Kentucky), John Blangero(The University of Texas Rio Grande Valley), Eric Boerwinkle(Baylor College of Medicine), Jiang He(Tulane University), Courtney G. Montgomery(Oklahoma Medical Research Foundation), D. C. Rao(Washington University in St. Louis), Jerome I. Rotter(UCLA Medical Center), Kent D. Taylor(UCLA Medical Center), Jennifer A. Brody(University of Washington), Yii‐Der Ida Chen(The Lundquist Institute), Lisa de las Fuentes(Washington University in St. Louis), Chii‐Min Hwu(National Yang Ming Chiao Tung University), Stephen S. Rich(University of Virginia), Ani Manichaikul(University of Virginia), Josyf C. Mychaleckyj(University of Virginia), Nicholette D. Palmer(Wake Forest University), Jennifer A. Smith(University of Michigan), Sharon L. R. Kardia(Institute for Social Research), Patricia A. Peyser(Institute for Social Research), Lawrence F. Bielak(Institute for Social Research), Timothy D. O’Connor(University of Maryland, Baltimore), Leslie S. Emery(University of Washington), TOPMed Population Genetics Working Group(Radboud University Nijmegen), Christian Gilissen(Inova Health System), Wendy S.W. Wong(Inova Health System), Peter V. Kharchenko(Brigham and Women's Hospital), Shamil Sunyaev(Brigham and Women's Hospital)
Science
August 12, 2021
10.1126/science.aba7408
Cited by 73Open Access
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Abstract

Biological mechanisms underlying human germline mutations remain largely unknown. We statistically decompose variation in the rate and spectra of mutations along the genome using volume-regularized nonnegative matrix factorization. The analysis of a sequencing dataset (TOPMed) reveals nine processes that explain the variation in mutation properties between loci. We provide a biological interpretation for seven of these processes. We associate one process with bulky DNA lesions that are resolved asymmetrically with respect to transcription and replication. Two processes track direction of replication fork and replication timing, respectively. We identify a mutagenic effect of active demethylation primarily acting in regulatory regions and a mutagenic effect of long interspersed nuclear elements. We localize a mutagenic process specific to oocytes from population sequencing data. This process appears transcriptionally asymmetric.

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