Origins and functional consequences of somatic mitochondrial DNA mutations in human cancer

ICGC Breast Cancer Group; ICGC Chronic Myeloid Disorders Group; ICGC Prostate Cancer Group

doi:10.7554/eLife.02935

Origins and functional consequences of somatic mitochondrial DNA mutations in human cancer

ICGC Breast Cancer Group, ICGC Chronic Myeloid Disorders Group, ICGC Prostate Cancer Group

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

295 Scopus citations

Abstract

Recent sequencing studies have extensively explored the somatic alterations present in the nuclear genomes of cancers. Although mitochondria control energy metabolism and apoptosis, the origins and impact of cancer-associated mutations in mtDNA are unclear. In this study, we analyzed somatic alterations in mtDNA from 1675 tumors. We identified 1907 somatic substitutions, which exhibited dramatic replicative strand bias, predominantly C > T and A > G on the mitochondrial heavy strand. This strand-asymmetric signature differs from those found in nuclear cancer genomes but matches the inferred germline process shaping primate mtDNA sequence content. A number of mtDNA mutations showed considerable heterogeneity across tumor types. Missense mutations were selectively neutral and often gradually drifted towards homoplasmy over time. In contrast, mutations resulting in protein truncation undergo negative selection and were almost exclusively heteroplasmic. Our findings indicate that the endogenous mutational mechanism has far greater impact than any other external mutagens in mitochondria and is fundamentally linked to mtDNA replication.

Original language	English (US)
Article number	e02935
Journal	eLife
Volume	3
DOIs	https://doi.org/10.7554/eLife.02935
State	Published - 2014
Externally published	Yes

Keywords

cancer genome
evolution
evolutionary biology
genomics
human
mitochondrial DNA
mutational signature
sequencing
somatic mutation

ASJC Scopus subject areas

General Neuroscience
General Biochemistry, Genetics and Molecular Biology
General Immunology and Microbiology

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10.7554/eLife.02935

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@article{08c5b62b22214a6c9fa964bae9642860,

title = "Origins and functional consequences of somatic mitochondrial DNA mutations in human cancer",

abstract = "Recent sequencing studies have extensively explored the somatic alterations present in the nuclear genomes of cancers. Although mitochondria control energy metabolism and apoptosis, the origins and impact of cancer-associated mutations in mtDNA are unclear. In this study, we analyzed somatic alterations in mtDNA from 1675 tumors. We identified 1907 somatic substitutions, which exhibited dramatic replicative strand bias, predominantly C > T and A > G on the mitochondrial heavy strand. This strand-asymmetric signature differs from those found in nuclear cancer genomes but matches the inferred germline process shaping primate mtDNA sequence content. A number of mtDNA mutations showed considerable heterogeneity across tumor types. Missense mutations were selectively neutral and often gradually drifted towards homoplasmy over time. In contrast, mutations resulting in protein truncation undergo negative selection and were almost exclusively heteroplasmic. Our findings indicate that the endogenous mutational mechanism has far greater impact than any other external mutagens in mitochondria and is fundamentally linked to mtDNA replication. ",

keywords = "cancer genome, evolution, evolutionary biology, genomics, human, mitochondrial DNA, mutational signature, sequencing, somatic mutation",

author = "{ICGC Breast Cancer Group} and {ICGC Chronic Myeloid Disorders Group} and {ICGC Prostate Cancer Group} and Ju, {Young S.eok} and Alexandrov, {Ludmil B.} and Moritz Gerstung and Inigo Martincorena and Serena Nik-Zainal and Manasa Ramakrishna and Davies, {Helen R.} and Elli Papaemmanuil and Gunes Gundem and Adam Shlien and Niccolo Bolli and Sam Behjati and Tarpey, {Patrick S.} and Jyoti Nangalia and Massie, {Charles E.} and Butler, {Adam P.} and Teague, {Jon W.} and Vassiliou, {George S.} and Green, {Anthony R.} and Du, {Ming Qing} and Ashwin Unnikrishnan and Pimanda, {John E.} and Teh, {Bin T.ean} and Nikhil Munshi and Mel Greaves and Paresh Vyas and El-Naggar, {Adel K.} and Tom Santarius and Collins, {V. Peter} and Richard Grundy and Taylor, {Jack A.} and Hayes, {D. Neil} and David Malkin and Foster, {Christopher S.} and Warren, {Anne Y.} and Whitaker, {Hayley C.} and Daniel Brewer and Rosalind Eeles and Colin Cooper and David Neal and Tapio Visakorpi and Isaacs, {William B.} and Bova, {G. Steven} and Flanagan, {Adrienne M.} and Futreal, {P. Andrew} and Lynch, {Andy G.} and Chinnery, {Patrick F.} and Ultan McDermott and Stratton, {Michael R.} and Campbell, {Peter J.}",

year = "2014",

doi = "10.7554/eLife.02935",

language = "English (US)",

volume = "3",

journal = "eLife",

issn = "2050-084X",

publisher = "eLife Sciences Publications",

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TY - JOUR

T1 - Origins and functional consequences of somatic mitochondrial DNA mutations in human cancer

AU - ICGC Breast Cancer Group

AU - ICGC Chronic Myeloid Disorders Group

AU - ICGC Prostate Cancer Group

AU - Ju, Young S.eok

AU - Alexandrov, Ludmil B.

AU - Gerstung, Moritz

AU - Martincorena, Inigo

AU - Nik-Zainal, Serena

AU - Ramakrishna, Manasa

AU - Davies, Helen R.

AU - Papaemmanuil, Elli

AU - Gundem, Gunes

AU - Shlien, Adam

AU - Bolli, Niccolo

AU - Behjati, Sam

AU - Tarpey, Patrick S.

AU - Nangalia, Jyoti

AU - Massie, Charles E.

AU - Butler, Adam P.

AU - Teague, Jon W.

AU - Vassiliou, George S.

AU - Green, Anthony R.

AU - Du, Ming Qing

AU - Unnikrishnan, Ashwin

AU - Pimanda, John E.

AU - Teh, Bin T.ean

AU - Munshi, Nikhil

AU - Greaves, Mel

AU - Vyas, Paresh

AU - El-Naggar, Adel K.

AU - Santarius, Tom

AU - Collins, V. Peter

AU - Grundy, Richard

AU - Taylor, Jack A.

AU - Hayes, D. Neil

AU - Malkin, David

AU - Foster, Christopher S.

AU - Warren, Anne Y.

AU - Whitaker, Hayley C.

AU - Brewer, Daniel

AU - Eeles, Rosalind

AU - Cooper, Colin

AU - Neal, David

AU - Visakorpi, Tapio

AU - Isaacs, William B.

AU - Bova, G. Steven

AU - Flanagan, Adrienne M.

AU - Futreal, P. Andrew

AU - Lynch, Andy G.

AU - Chinnery, Patrick F.

AU - McDermott, Ultan

AU - Stratton, Michael R.

AU - Campbell, Peter J.

PY - 2014

Y1 - 2014

N2 - Recent sequencing studies have extensively explored the somatic alterations present in the nuclear genomes of cancers. Although mitochondria control energy metabolism and apoptosis, the origins and impact of cancer-associated mutations in mtDNA are unclear. In this study, we analyzed somatic alterations in mtDNA from 1675 tumors. We identified 1907 somatic substitutions, which exhibited dramatic replicative strand bias, predominantly C > T and A > G on the mitochondrial heavy strand. This strand-asymmetric signature differs from those found in nuclear cancer genomes but matches the inferred germline process shaping primate mtDNA sequence content. A number of mtDNA mutations showed considerable heterogeneity across tumor types. Missense mutations were selectively neutral and often gradually drifted towards homoplasmy over time. In contrast, mutations resulting in protein truncation undergo negative selection and were almost exclusively heteroplasmic. Our findings indicate that the endogenous mutational mechanism has far greater impact than any other external mutagens in mitochondria and is fundamentally linked to mtDNA replication.

AB - Recent sequencing studies have extensively explored the somatic alterations present in the nuclear genomes of cancers. Although mitochondria control energy metabolism and apoptosis, the origins and impact of cancer-associated mutations in mtDNA are unclear. In this study, we analyzed somatic alterations in mtDNA from 1675 tumors. We identified 1907 somatic substitutions, which exhibited dramatic replicative strand bias, predominantly C > T and A > G on the mitochondrial heavy strand. This strand-asymmetric signature differs from those found in nuclear cancer genomes but matches the inferred germline process shaping primate mtDNA sequence content. A number of mtDNA mutations showed considerable heterogeneity across tumor types. Missense mutations were selectively neutral and often gradually drifted towards homoplasmy over time. In contrast, mutations resulting in protein truncation undergo negative selection and were almost exclusively heteroplasmic. Our findings indicate that the endogenous mutational mechanism has far greater impact than any other external mutagens in mitochondria and is fundamentally linked to mtDNA replication.

KW - cancer genome

KW - evolution

KW - evolutionary biology

KW - genomics

KW - human

KW - mitochondrial DNA

KW - mutational signature

KW - sequencing

KW - somatic mutation

UR - http://www.scopus.com/inward/record.url?scp=84994324806&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=84994324806&partnerID=8YFLogxK

U2 - 10.7554/eLife.02935

DO - 10.7554/eLife.02935

M3 - Article

C2 - 25271376

AN - SCOPUS:84994324806

SN - 2050-084X

VL - 3

JO - eLife

JF - eLife

M1 - e02935

ER -

Origins and functional consequences of somatic mitochondrial DNA mutations in human cancer

Abstract

Keywords

ASJC Scopus subject areas

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