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Sequencing and de novo assembly of 150 genomes from Denmark as a population reference

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DOI

  • Lasse Maretty, University of Copenhagen
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  • Jacob Malte Jensen
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  • Bent Petersen, Technical University of Denmark
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  • Jonas Andreas Sibbesen, University of Copenhagen
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  • Siyang Liu, BGI-Europe, Ole Maaløes Vej 3, 2200 Copenhagen, Denmark.
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  • Palle Villesen
  • Laurits Skov
  • Kirstine Christensen Belling, Technical University of Denmark
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  • Christian Theil Have, University of Copenhagen
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  • José M G Izarzugaza, Technical University of Denmark
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  • Marie Grosjean, Technical University of Denmark
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  • Jette Bork-Jensen, University of Copenhagen
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  • Jakob Grove
  • Thomas D Als
  • Shujia Huang, School of Bioscience and Biotechnology, South China University of Technology, Guangzhou 510006, China
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  • Yuqi Chang, BGI-Shenzhen, Shenzhen 518083, China
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  • Ruiqi Xu, BGI-Europe, Ole Maaløes Vej 3, 2200 Copenhagen, Denmark.
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  • Weijian Ye, BGI-Europe, Ole Maaløes Vej 3, 2200 Copenhagen, Denmark.
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  • Junhua Rao, BGI-Europe, Ole Maaløes Vej 3, 2200 Copenhagen, Denmark.
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  • Xiaosen Guo, University of Copenhagen
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  • Jihua Sun, University of Copenhagen
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  • Hongzhi Cao, BGI-Shenzhen, Shenzhen 518083, China
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  • Chen Ye, BGI-Shenzhen, Shenzhen 518083, China
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  • Johan van Beusekom, Technical University of Denmark
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  • Thomas Espeseth, K.G. Jebsen Centre for Psychosis Research, Norwegian Centre for Mental Disorders Research (NORMENT), Department of Clinical Science, University of Bergen, 5009, Bergen, Norway; Dr. Einar Martens Research Group for Biological Psychiatry, Center for Medical Genetics and Molecular Medicine, Haukeland University Hospital, 5021, Bergen, Norway.
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  • Esben Nørgaard Flindt, University of Copenhagen
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  • Rune M Friborg
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  • Anders E Halager
  • Stephanie Le Hellard, K.G. Jebsen Centre for Psychosis Research, Norwegian Centre for Mental Disorders Research (NORMENT), Department of Clinical Science, University of Bergen, 5009, Bergen, Norway; Dr. Einar Martens Research Group for Biological Psychiatry, Center for Medical Genetics and Molecular Medicine, Haukeland University Hospital, 5021, Bergen, Norway.
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  • Christina M Hultman, Karolinska Institutet
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  • Francesco Lescai, The Lundbeck Foundation Initiative for Integrative Psychiatric Research, iPSYCH, Risskov, Denmark ; Department of Biomedicine and Centre for Integrative Sequencing, iSEQ, University of Aarhus, Aarhus C, 8000 Denmark.
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  • Shengting Li
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  • Ole Lund, Technical University of Denmark
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  • Peter Løngren, Technical University of Denmark
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  • Thomas Mailund
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  • Maria Luisa Matey-Hernandez, Technical University of Denmark
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  • Ole Mors
  • Christian N S Pedersen
  • Thomas Sicheritz-Ponten, Technical University of Denmark
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  • Patrick F Sullivan, University of North Carolina
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  • Ali Syed, Technical University of Denmark
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  • David Westergaard, Technical University of Denmark
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  • Rachita Yadav, Technical University of Denmark
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  • Ning Li, BGI-Europe, Ole Maaløes Vej 3, 2200 Copenhagen, Denmark.
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  • Xun Xu, BGI-Shenzhen, Shenzhen 518083, China
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  • Torben Hansen, University of Copenhagen
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  • Anders Krogh, University of Copenhagen
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  • Lars Bolund
  • Thorkild I A Sørensen, University of Copenhagen
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  • Oluf Pedersen, University of Copenhagen
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  • Ramneek Gupta, Technical University of Denmark
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  • Simon Rasmussen, Technical University of Denmark
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  • Søren Besenbacher
  • Anders D Børglum
  • Jun Wang, The Lundbeck Foundation Initiative for Integrative Psychiatric Research, iPSYCH, Risskov, Denmark ; Department of Biomedicine and Centre for Integrative Sequencing, iSEQ, University of Aarhus, Aarhus C, 8000 Denmark., BGI-Shenzhen, Shenzhen 518083, China, University of Copenhagen
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  • Hans Eiberg, Department of Cellular and Molecular Medicine, University of Copenhagen, DK-2200 Copenhagen N, Denmark.
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  • Karsten Kristiansen, BGI-Shenzhen, Shenzhen 518083, China, University of Copenhagen
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  • Søren Brunak, University of Copenhagen
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  • Mikkel Heide Schierup

Hundreds of thousands of human genomes are now being sequenced to characterize genetic variation and use this information to augment association mapping studies of complex disorders and other phenotypic traits. Genetic variation is identified mainly by mapping short reads to the reference genome or by performing local assembly. However, these approaches are biased against discovery of structural variants and variation in the more complex parts of the genome. Hence, large-scale de novo assembly is needed. Here we show that it is possible to construct excellent de novo assemblies from high-coverage sequencing with mate-pair libraries extending up to 20 kilobases. We report de novo assemblies of 150 individuals (50 trios) from the GenomeDenmark project. The quality of these assemblies is similar to those obtained using the more expensive long-read technology. We use the assemblies to identify a rich set of structural variants including many novel insertions and demonstrate how this variant catalogue enables further deciphering of known association mapping signals. We leverage the assemblies to provide 100 completely resolved major histocompatibility complex haplotypes and to resolve major parts of the Y chromosome. Our study provides a regional reference genome that we expect will improve the power of future association mapping studies and hence pave the way for precision medicine initiatives, which now are being launched in many countries including Denmark.

Original languageEnglish
JournalNature
Volume548
Issue7665
Pages (from-to)87-91
Number of pages5
ISSN0028-0836
DOIs
Publication statusPublished - 3 Aug 2017

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  • Journal Article

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