Divergent mutational processes distinguish hypoxic and normoxic tumours

PCAWG Consortium

doi:10.1038/s41467-019-14052-x

Divergent mutational processes distinguish hypoxic and normoxic tumours

PCAWG Consortium

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

94 Scopus citations

Abstract

Many primary tumours have low levels of molecular oxygen (hypoxia), and hypoxic tumours respond poorly to therapy. Pan-cancer molecular hallmarks of tumour hypoxia remain poorly understood, with limited comprehension of its associations with specific mutational processes, non-coding driver genes and evolutionary features. Here, as part of the ICGC/TCGA Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium, which aggregated whole genome sequencing data from 2658 cancers across 38 tumour types, we quantify hypoxia in 1188 tumours spanning 27 cancer types. Elevated hypoxia associates with increased mutational load across cancer types, irrespective of underlying mutational class. The proportion of mutations attributed to several mutational signatures of unknown aetiology directly associates with the level of hypoxia, suggesting underlying mutational processes for these signatures. At the gene level, driver mutations in TP53, MYC and PTEN are enriched in hypoxic tumours, and mutations in PTEN interact with hypoxia to direct tumour evolutionary trajectories. Overall, hypoxia plays a critical role in shaping the genomic and evolutionary landscapes of cancer.

Original language	English
Article number	737
Journal	Nature communications
Volume	11
Issue number	1
DOIs	https://doi.org/10.1038/s41467-019-14052-x
State	Published - Dec 1 2020

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10.1038/s41467-019-14052-x

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@article{07bf31b57a004d4b9dcc7b119d1f26fe,

title = "Divergent mutational processes distinguish hypoxic and normoxic tumours",

abstract = "Many primary tumours have low levels of molecular oxygen (hypoxia), and hypoxic tumours respond poorly to therapy. Pan-cancer molecular hallmarks of tumour hypoxia remain poorly understood, with limited comprehension of its associations with specific mutational processes, non-coding driver genes and evolutionary features. Here, as part of the ICGC/TCGA Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium, which aggregated whole genome sequencing data from 2658 cancers across 38 tumour types, we quantify hypoxia in 1188 tumours spanning 27 cancer types. Elevated hypoxia associates with increased mutational load across cancer types, irrespective of underlying mutational class. The proportion of mutations attributed to several mutational signatures of unknown aetiology directly associates with the level of hypoxia, suggesting underlying mutational processes for these signatures. At the gene level, driver mutations in TP53, MYC and PTEN are enriched in hypoxic tumours, and mutations in PTEN interact with hypoxia to direct tumour evolutionary trajectories. Overall, hypoxia plays a critical role in shaping the genomic and evolutionary landscapes of cancer.",

author = "{PCAWG Consortium} and Vinayak Bhandari and Li, {Constance H.} and Bristow, {Robert G.} and Boutros, {Paul C.} and Aaltonen, {Lauri A.} and Federico Abascal and Adam Abeshouse and Hiroyuki Aburatani and Adams, {David J.} and Nishant Agrawal and Ahn, {Keun Soo} and Ahn, {Sung Min} and Hiroshi Aikata and Rehan Akbani and Akdemir, {Kadir C.} and Hikmat Al-Ahmadie and Al-Sedairy, {Sultan T.} and Fatima Al-Shahrour and Malik Alawi and Monique Albert and Kenneth Aldape and Alexandrov, {Ludmil B.} and Adrian Ally and Kathryn Alsop and Alvarez, {Eva G.} and Fernanda Amary and Amin, {Samirkumar B.} and Brice Aminou and Ole Ammerpohl and Anderson, {Matthew J.} and Yeng Ang and Davide Antonello and Pavana Anur and Samuel Aparicio and Appelbaum, {Elizabeth L.} and Yasuhito Arai and Axel Aretz and Koji Arihiro and Ariizumi, {Shun ichi} and Joshua Armenia and Laurent Arnould and Sylvia Asa and Yassen Assenov and Gurnit Atwal and Sietse Aukema and Auman, {J. Todd} and Aure, {Miriam R.R.} and Philip Awadalla and Marta Aymerich and Bader, {Gary D.} and Adrian Baez-Ortega and Bailey, {Matthew H.} and Bailey, {Peter J.} and Miruna Balasundaram and Saianand Balu and Pratiti Bandopadhayay and Banks, {Rosamonde E.} and Stefano Barbi and Barbour, {Andrew P.} and Jonathan Barenboim and Jill Barnholtz-Sloan and Hugh Barr and Elisabet Barrera and John Bartlett and Javier Bartolome and Claudio Bassi and Bathe, {Oliver F.} and Daniel Baumhoer and Prashant Bavi and Baylin, {Stephen B.} and Wojciech Bazant and Duncan Beardsmore and Beck, {Timothy A.} and Sam Behjati and Andreas Behren and Beifang Niu and Cindy Bell and Sergi Beltran and Christopher Benz and Andrew Berchuck and Bergmann, {Anke K.} and Bergstrom, {Erik N.} and Berman, {Benjamin P.} and Berney, {Daniel M.} and Bernhart, {Stephan H.} and Rameen Beroukhim and Mario Berrios and Samantha Bersani and Johanna Bertl and Miguel Betancourt and Vinayak Bhandari and Bhosle, {Shriram G.} and Biankin, {Andrew V.} and Matthias Bieg and Darell Bigner and Hans Binder and Ewan Birney and Michael Birrer and Biswas, {Nidhan K.} and Bodil Bjerkehagen and Tom Bodenheimer and Lori Boice and Giada Bonizzato and {De Bono}, {Johann S.} and Arnoud Boot and Bootwalla, {Moiz S.} and Ake Borg and Arndt Borkhardt and Boroevich, {Keith A.} and Ivan Borozan and Christoph Borst and Marcus Bosenberg and Mattia Bosio and Jacqueline Boultwood and Guillaume Bourque and Boutros, {Paul C.} and Bova, {G. Steven} and Bowen, {David T.} and Reanne Bowlby and Bowtell, {David D.L.} and Sandrine Boyault and Rich Boyce and Jeffrey Boyd and Alvis Brazma and Paul Brennan and Brewer, {Daniel S.} and Brinkman, {Arie B.} and Bristow, {Robert G.} and Broaddus, {Russell R.} and Brock, {Jane E.} and Malcolm Brock and Annegien Broeks and Brooks, {Angela N.} and Denise Brooks and Benedikt Brors and S{\o}ren Brunak and Bruxner, {Timothy J.C.} and Bruzos, {Alicia L.} and Alex Buchanan and Ivo Buchhalter and Christiane Buchholz and Susan Bullman and Hazel Burke and Birgit Burkhardt and Burns, {Kathleen H.} and John Busanovich and Bustamante, {Carlos D.} and Butler, {Adam P.} and Butte, {Atul J.} and Byrne, {Niall J.} and B{\o}rresen-Dale, {Anne Lise} and Caesar-Johnson, {Samantha J.} and Andy Cafferkey and Declan Cahill and Claudia Calabrese and Carlos Caldas and Fabien Calvo and Niedzica Camacho and Campbell, {Peter J.} and Elias Campo and Cinzia Cant{\`u} and Shaolong Cao and Carey, {Thomas E.} and Joana Carlevaro-Fita and Rebecca Carlsen and Ivana Cataldo and Mario Cazzola and Jonathan Cebon and Robert Cerfolio and Chadwick, {Dianne E.} and Dimple Chakravarty and Don Chalmers and Chan, {Calvin Wing Yiu} and Kin Chan and Michelle Chan-Seng-Yue and Chandan, {Vishal S.} and Chang, {David K.} and Chanock, {Stephen J.} and Chantrill, {Lorraine A.} and Aur{\'e}lien Chateigner and Nilanjan Chatterjee and Kazuaki Chayama and Chen, {Hsiao Wei} and Jieming Chen and Ken Chen and Yiwen Chen and Zhaohong Chen and Cherniack, {Andrew D.} and Jeremy Chien and Chiew, {Yoke Eng} and Chin, {Suet Feung} and Li Ding and Fulton, {Lucinda A.} and Fulton, {Robert S.} and Ramaswamy Govindan and Reyka Jayasinghe and Tim Ley and Miller, {Christopher A.} and David Mutch and Wendl, {Michael C.}",

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

year = "2020",

month = dec,

day = "1",

doi = "10.1038/s41467-019-14052-x",

language = "English",

volume = "11",

journal = "Nature communications",

issn = "2041-1723",

number = "1",

}

TY - JOUR

T1 - Divergent mutational processes distinguish hypoxic and normoxic tumours

AU - PCAWG Consortium

AU - Bhandari, Vinayak

AU - Li, Constance H.

AU - Bristow, Robert G.

AU - Boutros, Paul C.

AU - Aaltonen, Lauri A.

AU - Abascal, Federico

AU - Abeshouse, Adam

AU - Aburatani, Hiroyuki

AU - Adams, David J.

AU - Agrawal, Nishant

AU - Ahn, Keun Soo

AU - Ahn, Sung Min

AU - Aikata, Hiroshi

AU - Akbani, Rehan

AU - Akdemir, Kadir C.

AU - Al-Ahmadie, Hikmat

AU - Al-Sedairy, Sultan T.

AU - Al-Shahrour, Fatima

AU - Alawi, Malik

AU - Albert, Monique

AU - Aldape, Kenneth

AU - Alexandrov, Ludmil B.

AU - Ally, Adrian

AU - Alsop, Kathryn

AU - Alvarez, Eva G.

AU - Amary, Fernanda

AU - Amin, Samirkumar B.

AU - Aminou, Brice

AU - Ammerpohl, Ole

AU - Anderson, Matthew J.

AU - Ang, Yeng

AU - Antonello, Davide

AU - Anur, Pavana

AU - Aparicio, Samuel

AU - Appelbaum, Elizabeth L.

AU - Arai, Yasuhito

AU - Aretz, Axel

AU - Arihiro, Koji

AU - Ariizumi, Shun ichi

AU - Armenia, Joshua

AU - Arnould, Laurent

AU - Asa, Sylvia

AU - Assenov, Yassen

AU - Atwal, Gurnit

AU - Aukema, Sietse

AU - Auman, J. Todd

AU - Aure, Miriam R.R.

AU - Awadalla, Philip

AU - Aymerich, Marta

AU - Bader, Gary D.

AU - Baez-Ortega, Adrian

AU - Bailey, Matthew H.

AU - Bailey, Peter J.

AU - Balasundaram, Miruna

AU - Balu, Saianand

AU - Bandopadhayay, Pratiti

AU - Banks, Rosamonde E.

AU - Barbi, Stefano

AU - Barbour, Andrew P.

AU - Barenboim, Jonathan

AU - Barnholtz-Sloan, Jill

AU - Barr, Hugh

AU - Barrera, Elisabet

AU - Bartlett, John

AU - Bartolome, Javier

AU - Bassi, Claudio

AU - Bathe, Oliver F.

AU - Baumhoer, Daniel

AU - Bavi, Prashant

AU - Baylin, Stephen B.

AU - Bazant, Wojciech

AU - Beardsmore, Duncan

AU - Beck, Timothy A.

AU - Behjati, Sam

AU - Behren, Andreas

AU - Niu, Beifang

AU - Bell, Cindy

AU - Beltran, Sergi

AU - Benz, Christopher

AU - Berchuck, Andrew

AU - Bergmann, Anke K.

AU - Bergstrom, Erik N.

AU - Berman, Benjamin P.

AU - Berney, Daniel M.

AU - Bernhart, Stephan H.

AU - Beroukhim, Rameen

AU - Berrios, Mario

AU - Bersani, Samantha

AU - Bertl, Johanna

AU - Betancourt, Miguel

AU - Bhandari, Vinayak

AU - Bhosle, Shriram G.

AU - Biankin, Andrew V.

AU - Bieg, Matthias

AU - Bigner, Darell

AU - Binder, Hans

AU - Birney, Ewan

AU - Birrer, Michael

AU - Biswas, Nidhan K.

AU - Bjerkehagen, Bodil

AU - Bodenheimer, Tom

AU - Boice, Lori

AU - Bonizzato, Giada

AU - De Bono, Johann S.

AU - Boot, Arnoud

AU - Bootwalla, Moiz S.

AU - Borg, Ake

AU - Borkhardt, Arndt

AU - Boroevich, Keith A.

AU - Borozan, Ivan

AU - Borst, Christoph

AU - Bosenberg, Marcus

AU - Bosio, Mattia

AU - Boultwood, Jacqueline

AU - Bourque, Guillaume

AU - Boutros, Paul C.

AU - Bova, G. Steven

AU - Bowen, David T.

AU - Bowlby, Reanne

AU - Bowtell, David D.L.

AU - Boyault, Sandrine

AU - Boyce, Rich

AU - Boyd, Jeffrey

AU - Brazma, Alvis

AU - Brennan, Paul

AU - Brewer, Daniel S.

AU - Brinkman, Arie B.

AU - Bristow, Robert G.

AU - Broaddus, Russell R.

AU - Brock, Jane E.

AU - Brock, Malcolm

AU - Broeks, Annegien

AU - Brooks, Angela N.

AU - Brooks, Denise

AU - Brors, Benedikt

AU - Brunak, Søren

AU - Bruxner, Timothy J.C.

AU - Bruzos, Alicia L.

AU - Buchanan, Alex

AU - Buchhalter, Ivo

AU - Buchholz, Christiane

AU - Bullman, Susan

AU - Burke, Hazel

AU - Burkhardt, Birgit

AU - Burns, Kathleen H.

AU - Busanovich, John

AU - Bustamante, Carlos D.

AU - Butler, Adam P.

AU - Butte, Atul J.

AU - Byrne, Niall J.

AU - Børresen-Dale, Anne Lise

AU - Caesar-Johnson, Samantha J.

AU - Cafferkey, Andy

AU - Cahill, Declan

AU - Calabrese, Claudia

AU - Caldas, Carlos

AU - Calvo, Fabien

AU - Camacho, Niedzica

AU - Campbell, Peter J.

AU - Campo, Elias

AU - Cantù, Cinzia

AU - Cao, Shaolong

AU - Carey, Thomas E.

AU - Carlevaro-Fita, Joana

AU - Carlsen, Rebecca

AU - Cataldo, Ivana

AU - Cazzola, Mario

AU - Cebon, Jonathan

AU - Cerfolio, Robert

AU - Chadwick, Dianne E.

AU - Chakravarty, Dimple

AU - Chalmers, Don

AU - Chan, Calvin Wing Yiu

AU - Chan, Kin

AU - Chan-Seng-Yue, Michelle

AU - Chandan, Vishal S.

AU - Chang, David K.

AU - Chanock, Stephen J.

AU - Chantrill, Lorraine A.

AU - Chateigner, Aurélien

AU - Chatterjee, Nilanjan

AU - Chayama, Kazuaki

AU - Chen, Hsiao Wei

AU - Chen, Jieming

AU - Chen, Ken

AU - Chen, Yiwen

AU - Chen, Zhaohong

AU - Cherniack, Andrew D.

AU - Chien, Jeremy

AU - Chiew, Yoke Eng

AU - Chin, Suet Feung

AU - Ding, Li

AU - Fulton, Lucinda A.

AU - Fulton, Robert S.

AU - Govindan, Ramaswamy

AU - Jayasinghe, Reyka

AU - Ley, Tim

AU - Miller, Christopher A.

AU - Mutch, David

AU - Wendl, Michael C.

PY - 2020/12/1

Y1 - 2020/12/1

N2 - Many primary tumours have low levels of molecular oxygen (hypoxia), and hypoxic tumours respond poorly to therapy. Pan-cancer molecular hallmarks of tumour hypoxia remain poorly understood, with limited comprehension of its associations with specific mutational processes, non-coding driver genes and evolutionary features. Here, as part of the ICGC/TCGA Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium, which aggregated whole genome sequencing data from 2658 cancers across 38 tumour types, we quantify hypoxia in 1188 tumours spanning 27 cancer types. Elevated hypoxia associates with increased mutational load across cancer types, irrespective of underlying mutational class. The proportion of mutations attributed to several mutational signatures of unknown aetiology directly associates with the level of hypoxia, suggesting underlying mutational processes for these signatures. At the gene level, driver mutations in TP53, MYC and PTEN are enriched in hypoxic tumours, and mutations in PTEN interact with hypoxia to direct tumour evolutionary trajectories. Overall, hypoxia plays a critical role in shaping the genomic and evolutionary landscapes of cancer.

AB - Many primary tumours have low levels of molecular oxygen (hypoxia), and hypoxic tumours respond poorly to therapy. Pan-cancer molecular hallmarks of tumour hypoxia remain poorly understood, with limited comprehension of its associations with specific mutational processes, non-coding driver genes and evolutionary features. Here, as part of the ICGC/TCGA Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium, which aggregated whole genome sequencing data from 2658 cancers across 38 tumour types, we quantify hypoxia in 1188 tumours spanning 27 cancer types. Elevated hypoxia associates with increased mutational load across cancer types, irrespective of underlying mutational class. The proportion of mutations attributed to several mutational signatures of unknown aetiology directly associates with the level of hypoxia, suggesting underlying mutational processes for these signatures. At the gene level, driver mutations in TP53, MYC and PTEN are enriched in hypoxic tumours, and mutations in PTEN interact with hypoxia to direct tumour evolutionary trajectories. Overall, hypoxia plays a critical role in shaping the genomic and evolutionary landscapes of cancer.

UR - http://www.scopus.com/inward/record.url?scp=85079073682&partnerID=8YFLogxK

U2 - 10.1038/s41467-019-14052-x

DO - 10.1038/s41467-019-14052-x

M3 - Article

C2 - 32024819

AN - SCOPUS:85079073682

SN - 2041-1723

VL - 11

JO - Nature communications

JF - Nature communications

IS - 1

M1 - 737

ER -

Divergent mutational processes distinguish hypoxic and normoxic tumours

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