Landscape of multi-nucleotide variants in 125,748 human exomes and 15,708 genomes

doi:https://doi.org/10.1038/s41467-019-12438-5

Landscape of multi-nucleotide variants in 125,748 human exomes and 15,708 genomes

,

The Hebrew University of Jerusalem, University of Haifa

Research output: Contribution to journal › Article › peer-review

Abstract

Multi-nucleotide variants (MNVs), defined as two or more nearby variants existing on the same haplotype in an individual, are a clinically and biologically important class of genetic variation. However, existing tools typically do not accurately classify MNVs, and understanding of their mutational origins remains limited. Here, we systematically survey MNVs in 125,748 whole exomes and 15,708 whole genomes from the Genome Aggregation Database (gnomAD). We identify 1,792,248 MNVs across the genome with constituent variants falling within 2 bp distance of one another, including 18,756 variants with a novel combined effect on protein sequence. Finally, we estimate the relative impact of known mutational mechanisms - CpG deamination, replication error by polymerase zeta, and polymerase slippage at repeat junctions - on the generation of MNVs. Our results demonstrate the value of haplotype-aware variant annotation, and refine our understanding of genome-wide mutational mechanisms of MNVs.

Original language	English
Article number	2539
Journal	Nature Communications
Volume	11
Issue number	1
DOIs	https://doi.org/10.1038/s41467-019-12438-5
State	Published - 1 Dec 2020

All Science Journal Classification (ASJC) codes

General Chemistry
General Biochemistry,Genetics and Molecular Biology
General Physics and Astronomy

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https://doi.org/10.1038/s41467-019-12438-5

Cite this

@article{039f88c5d31f4f03b5df3845df48b7d0,

title = "Landscape of multi-nucleotide variants in 125,748 human exomes and 15,708 genomes",

abstract = "Multi-nucleotide variants (MNVs), defined as two or more nearby variants existing on the same haplotype in an individual, are a clinically and biologically important class of genetic variation. However, existing tools typically do not accurately classify MNVs, and understanding of their mutational origins remains limited. Here, we systematically survey MNVs in 125,748 whole exomes and 15,708 whole genomes from the Genome Aggregation Database (gnomAD). We identify 1,792,248 MNVs across the genome with constituent variants falling within 2 bp distance of one another, including 18,756 variants with a novel combined effect on protein sequence. Finally, we estimate the relative impact of known mutational mechanisms - CpG deamination, replication error by polymerase zeta, and polymerase slippage at repeat junctions - on the generation of MNVs. Our results demonstrate the value of haplotype-aware variant annotation, and refine our understanding of genome-wide mutational mechanisms of MNVs.",

author = "Qingbo Wang and Emma Pierce-Hoffman and Cummings, {Beryl B.} and Jessica Alf{\"o}ldi and Francioli, {Laurent C.} and Gauthier, {Laura D.} and Hill, {Andrew J.} and O{\textquoteright}Donnell-Luria, {Anne H.} and Armean, {Irina M.} and Eric Banks and Louis Bergelson and Kristian Cibulskis and Collins, {Ryan L.} and Connolly, {Kristen M.} and Miguel Covarrubias and Daly, {Mark J.} and Stacey Donnelly and Yossi Farjoun and Steven Ferriera and Stacey Gabriel and Jeff Gentry and Namrata Gupta and Thibault Jeandet and Diane Kaplan and Laricchia, {Kristen M.} and Christopher Llanwarne and Minikel, {Eric V.} and Ruchi Munshi and Neale, {Benjamin M.} and Sam Novod and Nikelle Petrillo and Timothy Poterba and David Roazen and Valentin Ruano-Rubio and Andrea Saltzman and Samocha, {Kaitlin E.} and Molly Schleicher and Cotton Seed and Matthew Solomonson and Jose Soto and Grace Tiao and Kathleen Tibbetts and Charlotte Tolonen and Christopher Vittal and Gordon Wade and Arcturus Wang and Ware, {James S.} and Watts, {Nicholas A.} and Ben Weisburd and Dan Turner and Gil Atzmon",

note = "Publisher Copyright: {\textcopyright} 2020, The Author(s).",

year = "2020",

month = dec,

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doi = "https://doi.org/10.1038/s41467-019-12438-5",

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T1 - Landscape of multi-nucleotide variants in 125,748 human exomes and 15,708 genomes

AU - Wang, Qingbo

AU - Pierce-Hoffman, Emma

AU - Cummings, Beryl B.

AU - Alföldi, Jessica

AU - Francioli, Laurent C.

AU - Gauthier, Laura D.

AU - Hill, Andrew J.

AU - O’Donnell-Luria, Anne H.

AU - Armean, Irina M.

AU - Banks, Eric

AU - Bergelson, Louis

AU - Cibulskis, Kristian

AU - Collins, Ryan L.

AU - Connolly, Kristen M.

AU - Covarrubias, Miguel

AU - Daly, Mark J.

AU - Donnelly, Stacey

AU - Farjoun, Yossi

AU - Ferriera, Steven

AU - Gabriel, Stacey

AU - Gentry, Jeff

AU - Gupta, Namrata

AU - Jeandet, Thibault

AU - Kaplan, Diane

AU - Laricchia, Kristen M.

AU - Llanwarne, Christopher

AU - Minikel, Eric V.

AU - Munshi, Ruchi

AU - Neale, Benjamin M.

AU - Novod, Sam

AU - Petrillo, Nikelle

AU - Poterba, Timothy

AU - Roazen, David

AU - Ruano-Rubio, Valentin

AU - Saltzman, Andrea

AU - Samocha, Kaitlin E.

AU - Schleicher, Molly

AU - Seed, Cotton

AU - Solomonson, Matthew

AU - Soto, Jose

AU - Tiao, Grace

AU - Tibbetts, Kathleen

AU - Tolonen, Charlotte

AU - Vittal, Christopher

AU - Wade, Gordon

AU - Wang, Arcturus

AU - Ware, James S.

AU - Watts, Nicholas A.

AU - Weisburd, Ben

AU - Turner, Dan

AU - Atzmon, Gil

PY - 2020/12/1

Y1 - 2020/12/1

N2 - Multi-nucleotide variants (MNVs), defined as two or more nearby variants existing on the same haplotype in an individual, are a clinically and biologically important class of genetic variation. However, existing tools typically do not accurately classify MNVs, and understanding of their mutational origins remains limited. Here, we systematically survey MNVs in 125,748 whole exomes and 15,708 whole genomes from the Genome Aggregation Database (gnomAD). We identify 1,792,248 MNVs across the genome with constituent variants falling within 2 bp distance of one another, including 18,756 variants with a novel combined effect on protein sequence. Finally, we estimate the relative impact of known mutational mechanisms - CpG deamination, replication error by polymerase zeta, and polymerase slippage at repeat junctions - on the generation of MNVs. Our results demonstrate the value of haplotype-aware variant annotation, and refine our understanding of genome-wide mutational mechanisms of MNVs.

AB - Multi-nucleotide variants (MNVs), defined as two or more nearby variants existing on the same haplotype in an individual, are a clinically and biologically important class of genetic variation. However, existing tools typically do not accurately classify MNVs, and understanding of their mutational origins remains limited. Here, we systematically survey MNVs in 125,748 whole exomes and 15,708 whole genomes from the Genome Aggregation Database (gnomAD). We identify 1,792,248 MNVs across the genome with constituent variants falling within 2 bp distance of one another, including 18,756 variants with a novel combined effect on protein sequence. Finally, we estimate the relative impact of known mutational mechanisms - CpG deamination, replication error by polymerase zeta, and polymerase slippage at repeat junctions - on the generation of MNVs. Our results demonstrate the value of haplotype-aware variant annotation, and refine our understanding of genome-wide mutational mechanisms of MNVs.

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U2 - https://doi.org/10.1038/s41467-019-12438-5

DO - https://doi.org/10.1038/s41467-019-12438-5

M3 - مقالة

C2 - 32461613

SN - 2041-1723

VL - 11

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 2539

ER -

Landscape of multi-nucleotide variants in 125,748 human exomes and 15,708 genomes

Abstract

All Science Journal Classification (ASJC) codes

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