Pathogenic Germline Variants in 10,389 Adult Cancers

The Cancer Genome Atlas Research Network

doi:10.1016/j.cell.2018.03.039

Pathogenic Germline Variants in 10,389 Adult Cancers

The Cancer Genome Atlas Research Network

电子与信息学部

Washington University St. Louis
Baylor College of Medicine
Ontario Institute for Cancer Research
Institute for Systems Biology
Broad Institute
University of Toronto
Inc.
University of Texas MD Anderson Cancer Center
Mayo Clinic Rochester, MN
Kuwait University
Princeton University
Wake Forest University
Baylor Genetics, LLC

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664 引用（Scopus）

摘要

We conducted the largest investigation of predisposition variants in cancer to date, discovering 853 pathogenic or likely pathogenic variants in 8% of 10,389 cases from 33 cancer types. Twenty-one genes showed single or cross-cancer associations, including novel associations of SDHA in melanoma and PALB2 in stomach adenocarcinoma. The 659 predisposition variants and 18 additional large deletions in tumor suppressors, including ATM, BRCA1, and NF1, showed low gene expression and frequent (43%) loss of heterozygosity or biallelic two-hit events. We also discovered 33 such variants in oncogenes, including missenses in MET, RET, and PTPN11 associated with high gene expression. We nominated 47 additional predisposition variants from prioritized VUSs supported by multiple evidences involving case-control frequency, loss of heterozygosity, expression effect, and co-localization with mutations and modified residues. Our integrative approach links rare predisposition variants to functional consequences, informing future guidelines of variant classification and germline genetic testing in cancer. A pan-cancer analysis identifies hundreds of predisposing germline variants.

源语言	英语
页（从-至）	355-370.e14
期刊	Cell
卷	173
期	2
DOI	https://doi.org/10.1016/j.cell.2018.03.039
出版状态	已出版 - 5 4月 2018

联合国可持续发展目标

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可持续发展目标 3 良好健康与福祉

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10.1016/j.cell.2018.03.039

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@article{a2f55c40416c4cb3b800e4f8e26e2438,

title = "Pathogenic Germline Variants in 10,389 Adult Cancers",

abstract = "We conducted the largest investigation of predisposition variants in cancer to date, discovering 853 pathogenic or likely pathogenic variants in 8\% of 10,389 cases from 33 cancer types. Twenty-one genes showed single or cross-cancer associations, including novel associations of SDHA in melanoma and PALB2 in stomach adenocarcinoma. The 659 predisposition variants and 18 additional large deletions in tumor suppressors, including ATM, BRCA1, and NF1, showed low gene expression and frequent (43\%) loss of heterozygosity or biallelic two-hit events. We also discovered 33 such variants in oncogenes, including missenses in MET, RET, and PTPN11 associated with high gene expression. We nominated 47 additional predisposition variants from prioritized VUSs supported by multiple evidences involving case-control frequency, loss of heterozygosity, expression effect, and co-localization with mutations and modified residues. Our integrative approach links rare predisposition variants to functional consequences, informing future guidelines of variant classification and germline genetic testing in cancer. A pan-cancer analysis identifies hundreds of predisposing germline variants.",

keywords = "LOH, cancer predisposition, germline and somatic genomes, variant pathogenicity",

author = "\{The Cancer Genome Atlas Research Network\} and Huang, \{Kuan lin\} and Mashl, \{R. Jay\} and Yige Wu and Ritter, \{Deborah I.\} and Jiayin Wang and Clara Oh and Marta Paczkowska and Sheila Reynolds and Wyczalkowski, \{Matthew A.\} and Ninad Oak and Scott, \{Adam D.\} and Michal Krassowski and Cherniack, \{Andrew D.\} and Houlahan, \{Kathleen E.\} and Reyka Jayasinghe and Wang, \{Liang Bo\} and Zhou, \{Daniel Cui\} and Di Liu and Song Cao and Kim, \{Young Won\} and Amanda Koire and McMichael, \{Joshua F.\} and Vishwanathan Hucthagowder and Kim, \{Tae Beom\} and Abigail Hahn and Chen Wang and McLellan, \{Michael D.\} and Fahd Al-Mulla and Johnson, \{Kimberly J.\} and Caesar-Johnson, \{Samantha J.\} and Demchok, \{John A.\} and Ina Felau and Melpomeni Kasapi and Ferguson, \{Martin L.\} and Hutter, \{Carolyn M.\} and Sofia, \{Heidi J.\} and Roy Tarnuzzer and Zhining Wang and Liming Yang and Zenklusen, \{Jean C.\} and Zhang, \{Jiashan (Julia)\} and Sudha Chudamani and Jia Liu and Laxmi Lolla and Rashi Naresh and Todd Pihl and Qiang Sun and Yunhu Wan and Ye Wu and Juok Cho",

note = "Publisher Copyright: {\textcopyright} 2018 The Authors",

year = "2018",

month = apr,

day = "5",

doi = "10.1016/j.cell.2018.03.039",

language = "英语",

volume = "173",

pages = "355--370.e14",

journal = "Cell",

issn = "0092-8674",

publisher = "Elsevier B.V.",

number = "2",

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TY - JOUR

T1 - Pathogenic Germline Variants in 10,389 Adult Cancers

AU - The Cancer Genome Atlas Research Network

AU - Huang, Kuan lin

AU - Mashl, R. Jay

AU - Wu, Yige

AU - Ritter, Deborah I.

AU - Wang, Jiayin

AU - Oh, Clara

AU - Paczkowska, Marta

AU - Reynolds, Sheila

AU - Wyczalkowski, Matthew A.

AU - Oak, Ninad

AU - Scott, Adam D.

AU - Krassowski, Michal

AU - Cherniack, Andrew D.

AU - Houlahan, Kathleen E.

AU - Jayasinghe, Reyka

AU - Wang, Liang Bo

AU - Zhou, Daniel Cui

AU - Liu, Di

AU - Cao, Song

AU - Kim, Young Won

AU - Koire, Amanda

AU - McMichael, Joshua F.

AU - Hucthagowder, Vishwanathan

AU - Kim, Tae Beom

AU - Hahn, Abigail

AU - Wang, Chen

AU - McLellan, Michael D.

AU - Al-Mulla, Fahd

AU - Johnson, Kimberly J.

AU - Caesar-Johnson, Samantha J.

AU - Demchok, John A.

AU - Felau, Ina

AU - Kasapi, Melpomeni

AU - Ferguson, Martin L.

AU - Hutter, Carolyn M.

AU - Sofia, Heidi J.

AU - Tarnuzzer, Roy

AU - Wang, Zhining

AU - Yang, Liming

AU - Zenklusen, Jean C.

AU - Zhang, Jiashan (Julia)

AU - Chudamani, Sudha

AU - Liu, Jia

AU - Lolla, Laxmi

AU - Naresh, Rashi

AU - Pihl, Todd

AU - Sun, Qiang

AU - Wan, Yunhu

AU - Wu, Ye

AU - Cho, Juok

PY - 2018/4/5

Y1 - 2018/4/5

N2 - We conducted the largest investigation of predisposition variants in cancer to date, discovering 853 pathogenic or likely pathogenic variants in 8% of 10,389 cases from 33 cancer types. Twenty-one genes showed single or cross-cancer associations, including novel associations of SDHA in melanoma and PALB2 in stomach adenocarcinoma. The 659 predisposition variants and 18 additional large deletions in tumor suppressors, including ATM, BRCA1, and NF1, showed low gene expression and frequent (43%) loss of heterozygosity or biallelic two-hit events. We also discovered 33 such variants in oncogenes, including missenses in MET, RET, and PTPN11 associated with high gene expression. We nominated 47 additional predisposition variants from prioritized VUSs supported by multiple evidences involving case-control frequency, loss of heterozygosity, expression effect, and co-localization with mutations and modified residues. Our integrative approach links rare predisposition variants to functional consequences, informing future guidelines of variant classification and germline genetic testing in cancer. A pan-cancer analysis identifies hundreds of predisposing germline variants.

AB - We conducted the largest investigation of predisposition variants in cancer to date, discovering 853 pathogenic or likely pathogenic variants in 8% of 10,389 cases from 33 cancer types. Twenty-one genes showed single or cross-cancer associations, including novel associations of SDHA in melanoma and PALB2 in stomach adenocarcinoma. The 659 predisposition variants and 18 additional large deletions in tumor suppressors, including ATM, BRCA1, and NF1, showed low gene expression and frequent (43%) loss of heterozygosity or biallelic two-hit events. We also discovered 33 such variants in oncogenes, including missenses in MET, RET, and PTPN11 associated with high gene expression. We nominated 47 additional predisposition variants from prioritized VUSs supported by multiple evidences involving case-control frequency, loss of heterozygosity, expression effect, and co-localization with mutations and modified residues. Our integrative approach links rare predisposition variants to functional consequences, informing future guidelines of variant classification and germline genetic testing in cancer. A pan-cancer analysis identifies hundreds of predisposing germline variants.

KW - LOH

KW - cancer predisposition

KW - germline and somatic genomes

KW - variant pathogenicity

UR - https://www.scopus.com/pages/publications/85044578706

U2 - 10.1016/j.cell.2018.03.039

DO - 10.1016/j.cell.2018.03.039

M3 - 文章

C2 - 29625052

AN - SCOPUS:85044578706

SN - 0092-8674

VL - 173

SP - 355-370.e14

JO - Cell

JF - Cell

IS - 2

ER -

Pathogenic Germline Variants in 10,389 Adult Cancers

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