Search CORE

2 research outputs found

Characteristics of de novo structural changes in the human genome

Small insertions and deletions (indels) and large structural variations (SVs) are major contributors to human genetic diversity and disease. However, mutation rates and characteristics of de novo indels and SVs in the general population have remained largely unexplored. We report 332 validated de novo structural changes identified in whole genomes of 250 families, including complex indels, retrotransposon insertions, and interchromosomal events. These data indicate a mutation rate of 2.94 indels (120 bp) and 0.16 SVs (>20 bp) per generation. De novo structural changes affect on average 4.1 kbp of genomic sequence and 29 coding bases per generation, which is 91 and 52 times more nucleotides than de novo substitutions, respectively. This contrasts with the equal genomic footprint of inherited SVs and substitutions. An excess of structural changes originated on paternal haplotypes. Additionally, we observed a nonuniform distribution of de novo SVs across offspring. These results reveal the importance of different mutational mechanisms to changes in human genome structure across generations

Erasmus University Digital Repository

A high-quality human reference panel reveals the complexity and distribution of genomic structural variants

Author: Abdellaoui A. (Abdel)
Amin N. (Najaf)
Baaijens J.A. (Jasmijn)
Bakker P.I.W. (Paul) de
Beekman M. (Marian)
Boomsma D.I. (Dorret)
Bot J. (Jan)
Bovenberg J.A. (Jasper)
Byelas G. (George)
Cao H. (Hongzhi)
Cao J.S. (Jeremy Sujie)
Cao R. (Rui)
Chen R. (Ruoyan)
Coe B.P. (Bradley)
Craen A.J.M. (Anton) de
Deelen P. (Patrick)
Dijk F. (Freerk) van
Dijkstra L.J. (Louis)
Dijkstra M. (Martijn)
Du Y. (Yuanping)
Duijn C.M. (Cornelia) van
Dunnen J.T. (Johan) den
Eichler E.E. (Evan)
Enckevort D. (David) van
Estrada K. (Karol)
Francioli L.C. (Laurent)
Guryev V. (Victor)
Handsaker R.E. (Robert)
Hehir-Kwa J.Y. (Jayne)
Hofman A. (Albert)
Hormozdiari F. (Fereydoun)
Hottenga J.-J. (Jouke-Jan)
Kanterakis A. (Alexandros)
Karssen L.C. (Lennart)
Kattenberg V.M. (Mathijs)
Kloosterman W.P. (Wigard)
Knijff P. (Peter) de
Ko A. (Arthur)
Koval V. (Vyacheslav)
Lameijer E.-W. (Eric-Wubbo)
Laros J.F.J. (Jeroen)
Ligt J. (Joep) de
Marschall T. (Tobias)
McCarroll S.A. (Steven)
Mei H. (Hailiang)
Neerincx P.B.T. (Pieter)
Nijman I.J. (Isaac)
Ommen G.-J.B. (Gert-Jan) van
Platteel M. (Mathieu)
Renkens I. (Ivo)
Rivadeneira F. (Fernando)
Santcroos M. (Mark)
Schaik B.D.C. (Barbera) van
Schönhuth A. (Alexander)
Slagboom P.E. (Eline)
Sudmant P. (Peter)
Sun Y. (Yushen)
Swertz M.A. (Morris)
Thung (), D.T. (Djie Tjwan)
Uitterlinden A.G. (André)
van Leeuwen E.M. (Elisa)
Vermaat M. (Martijn)
Wardenaar R. (René)
Wijmenga C. (Cisca)
Willemsen G. (Gonneke)
Wolffenbuttel B. (Bruce)
Ye K. (Kai)
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 06/10/2016
Field of study

Structural variation (SV) represents a major source of differences between individual human genomes and has been linked to disease phenotypes. However, the majority of studies provide neither a global view of the full spectrum of these variants nor integrate them into reference panels of genetic variation. Here, we analyse whole genome sequencing data of 769 individuals from 250 Dutch families, and provide a haplotype-resolved map of 1.9 million genome variants across 9 different variant classes, including novel forms of complex indels, and retrotransposition-mediated insertions of mobile elements and processed RNAs. A large proportion are previously under reported variants sized between 21 and 100 bp. We detect 4 megabases of novel sequence, encoding 11 new transcripts. Finally, we show 191 known, trait-associated SNPs to be in strong linkage disequilibrium with SVs and demonstrate that our panel facilitates accurate imputation of SVs in unrelated individuals

CWI's Institutional Repository