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Whole-genome sequence variation, population structure and demographic history of the Dutch population

Authors :
Francioli, L.C.
Menelaou, A.
Pulit, S.L.
Dijk, F. van
Palamara, P.F.
Elbers, C.C.
Neerincx, P.B.
Ye, K.
Guryev, V.
Kloosterman, W.P.
Deelen, P.
Abdellaoui, A.
Leeuwen, E.M. van
Oven, M. van
Vermaat, M.
Li, M.
Laros, J.F.
Karssen, L.C.
Kanterakis, A.
Amin, N.
Hottenga, J.J.
Lameijer, E.W.
Kattenberg, M.
Dijkstra, M.
Byelas, H.
Setten, J. van
Schaik, B.D. van
Bot, J.
Nijman, I.J.
Renkens, I.
Marschall, T.
Schönhuth, A.
Hehir-Kwa, J.Y.
Handsaker, R.E.
Polak, P.
Sohail, M.
Vuzman, D.
Hormozdiari, F.
Enckevort, D. van
Mei, H.
Koval, V.
Moed, M.H.
Velde, K.J. van der
Rivadeneira, F.
Estrada, K.
Medina-Gomez, C.
Isaacs, A.
McCarroll, S.A.
Beekman, M.
Craen, A.J. de
Suchiman, H.E.
Hofman, A.
Oostra, B.
Uitterlinden, A.G.
Willemsen, G.
Platteel, M.
Veldink, J.H.
Berg, L.H. van den
Pitts, S.J.
Potluri, S.
Sundar, P.
Cox, D.R.
Sunyaev, S.R.
Dunnen, J.T. den
Stoneking, M.
Knijff, P. de
Kayser, M.
Li, Q.
Li, Y.
Du, Y.
Chen, R.
Cao, H.
Li, N.
Cao, S.
Wang, J
Bovenberg, J.A.
Pe'er, I.
Slagboom, P.E.
Duijn, C.M. van
Boomsma, D.I.
Ommen, G.J. van
Bakker, P.I. de
Swertz, M.A.
Wijmenga, C.
Francioli, L.C.
Menelaou, A.
Pulit, S.L.
Dijk, F. van
Palamara, P.F.
Elbers, C.C.
Neerincx, P.B.
Ye, K.
Guryev, V.
Kloosterman, W.P.
Deelen, P.
Abdellaoui, A.
Leeuwen, E.M. van
Oven, M. van
Vermaat, M.
Li, M.
Laros, J.F.
Karssen, L.C.
Kanterakis, A.
Amin, N.
Hottenga, J.J.
Lameijer, E.W.
Kattenberg, M.
Dijkstra, M.
Byelas, H.
Setten, J. van
Schaik, B.D. van
Bot, J.
Nijman, I.J.
Renkens, I.
Marschall, T.
Schönhuth, A.
Hehir-Kwa, J.Y.
Handsaker, R.E.
Polak, P.
Sohail, M.
Vuzman, D.
Hormozdiari, F.
Enckevort, D. van
Mei, H.
Koval, V.
Moed, M.H.
Velde, K.J. van der
Rivadeneira, F.
Estrada, K.
Medina-Gomez, C.
Isaacs, A.
McCarroll, S.A.
Beekman, M.
Craen, A.J. de
Suchiman, H.E.
Hofman, A.
Oostra, B.
Uitterlinden, A.G.
Willemsen, G.
Platteel, M.
Veldink, J.H.
Berg, L.H. van den
Pitts, S.J.
Potluri, S.
Sundar, P.
Cox, D.R.
Sunyaev, S.R.
Dunnen, J.T. den
Stoneking, M.
Knijff, P. de
Kayser, M.
Li, Q.
Li, Y.
Du, Y.
Chen, R.
Cao, H.
Li, N.
Cao, S.
Wang, J
Bovenberg, J.A.
Pe'er, I.
Slagboom, P.E.
Duijn, C.M. van
Boomsma, D.I.
Ommen, G.J. van
Bakker, P.I. de
Swertz, M.A.
Wijmenga, C.
Source :
Nature Genetics; 818; 825; 1061-4036; 8; 46; ~Nature Genetics~818~825~~~1061-4036~8~46~~
Publication Year :
2014

Abstract

Contains fulltext : 137213.pdf (publisher's version ) (Closed access)<br />Whole-genome sequencing enables complete characterization of genetic variation, but geographic clustering of rare alleles demands many diverse populations be studied. Here we describe the Genome of the Netherlands (GoNL) Project, in which we sequenced the whole genomes of 250 Dutch parent-offspring families and constructed a haplotype map of 20.4 million single-nucleotide variants and 1.2 million insertions and deletions. The intermediate coverage ( approximately 13x) and trio design enabled extensive characterization of structural variation, including midsize events (30-500 bp) previously poorly catalogued and de novo mutations. We demonstrate that the quality of the haplotypes boosts imputation accuracy in independent samples, especially for lower frequency alleles. Population genetic analyses demonstrate fine-scale structure across the country and support multiple ancient migrations, consistent with historical changes in sea level and flooding. The GoNL Project illustrates how single-population whole-genome sequencing can provide detailed characterization of genetic variation and may guide the design of future population studies.

Details

Database :
OAIster
Journal :
Nature Genetics; 818; 825; 1061-4036; 8; 46; ~Nature Genetics~818~825~~~1061-4036~8~46~~
Publication Type :
Electronic Resource
Accession number :
edsoai.on1284049397
Document Type :
Electronic Resource