Simultaneous DNA and RNA mapping of somatic mitochondrial mutations across diverse human cancers

James B. Stewart; Babak Alaei-Mahabadi; Sabarinathan Radhakrishnan; Tore Samuelsson; Jan Gorodkin; Claes M Gustafsson; Erik Larsson

doi:10.1371/journal.pgen.1005333

Simultaneous DNA and RNA mapping of somatic mitochondrial mutations across diverse human cancers

James B. Stewart, Babak Alaei-Mahabadi, Sabarinathan Radhakrishnan, Tore Samuelsson, Jan Gorodkin, Claes M Gustafsson, Erik Larsson

56 Citationer (Scopus)

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Abstract

Somatic mutations in the nuclear genome are required for tumor formation, but the functional consequences of somatic mitochondrial DNA (mtDNA) mutations are less understood. Here we identify somatic mtDNA mutations across 527 tumors and 14 cancer types, using an approach that takes advantage of evidence from both genomic and transcriptomic sequencing. We find that there is selective pressure against deleterious coding mutations, supporting that functional mitochondria are required in tumor cells, and also observe a strong mutational strand bias, compatible with endogenous replication-coupled errors as the major source of mutations. Interestingly, while allelic ratios in general were consistent in RNA compared to DNA, some mutations in tRNAs displayed strong allelic imbalances caused by accumulation of unprocessed tRNA precursors. The effect was explained by altered secondary structure, demonstrating that correct tRNA folding is a major determinant for processing of polycistronic mitochondrial transcripts. Additionally, the data suggest that tRNA clusters are preferably processed in the 3' to 5' direction. Our study gives insights into mtDNA function in cancer and answers questions regarding mitochondrial tRNA biogenesis that are difficult to address in controlled experimental systems.

Originalsprog	Engelsk
Artikelnummer	e1005333
Tidsskrift	P L o S Genetics
Vol/bind	11
Udgave nummer	6
Antal sider	15
ISSN	1553-7390
DOI	https://doi.org/10.1371/journal.pgen.1005333
Status	Udgivet - 30 jun. 2015

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Simultaneous DNA and RNA mapping of somatic mitochondrial mutations across diverse human cancersForlagets udgivne version, 1,71 MB

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title = "Simultaneous DNA and RNA mapping of somatic mitochondrial mutations across diverse human cancers",

abstract = "Somatic mutations in the nuclear genome are required for tumor formation, but the functional consequences of somatic mitochondrial DNA (mtDNA) mutations are less understood. Here we identify somatic mtDNA mutations across 527 tumors and 14 cancer types, using an approach that takes advantage of evidence from both genomic and transcriptomic sequencing. We find that there is selective pressure against deleterious coding mutations, supporting that functional mitochondria are required in tumor cells, and also observe a strong mutational strand bias, compatible with endogenous replication-coupled errors as the major source of mutations. Interestingly, while allelic ratios in general were consistent in RNA compared to DNA, some mutations in tRNAs displayed strong allelic imbalances caused by accumulation of unprocessed tRNA precursors. The effect was explained by altered secondary structure, demonstrating that correct tRNA folding is a major determinant for processing of polycistronic mitochondrial transcripts. Additionally, the data suggest that tRNA clusters are preferably processed in the 3' to 5' direction. Our study gives insights into mtDNA function in cancer and answers questions regarding mitochondrial tRNA biogenesis that are difficult to address in controlled experimental systems.",

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T1 - Simultaneous DNA and RNA mapping of somatic mitochondrial mutations across diverse human cancers

AU - Stewart, James B.

AU - Alaei-Mahabadi, Babak

AU - Radhakrishnan, Sabarinathan

AU - Samuelsson, Tore

AU - Gorodkin, Jan

AU - Gustafsson, Claes M

AU - Larsson, Erik

PY - 2015/6/30

Y1 - 2015/6/30

N2 - Somatic mutations in the nuclear genome are required for tumor formation, but the functional consequences of somatic mitochondrial DNA (mtDNA) mutations are less understood. Here we identify somatic mtDNA mutations across 527 tumors and 14 cancer types, using an approach that takes advantage of evidence from both genomic and transcriptomic sequencing. We find that there is selective pressure against deleterious coding mutations, supporting that functional mitochondria are required in tumor cells, and also observe a strong mutational strand bias, compatible with endogenous replication-coupled errors as the major source of mutations. Interestingly, while allelic ratios in general were consistent in RNA compared to DNA, some mutations in tRNAs displayed strong allelic imbalances caused by accumulation of unprocessed tRNA precursors. The effect was explained by altered secondary structure, demonstrating that correct tRNA folding is a major determinant for processing of polycistronic mitochondrial transcripts. Additionally, the data suggest that tRNA clusters are preferably processed in the 3' to 5' direction. Our study gives insights into mtDNA function in cancer and answers questions regarding mitochondrial tRNA biogenesis that are difficult to address in controlled experimental systems.

AB - Somatic mutations in the nuclear genome are required for tumor formation, but the functional consequences of somatic mitochondrial DNA (mtDNA) mutations are less understood. Here we identify somatic mtDNA mutations across 527 tumors and 14 cancer types, using an approach that takes advantage of evidence from both genomic and transcriptomic sequencing. We find that there is selective pressure against deleterious coding mutations, supporting that functional mitochondria are required in tumor cells, and also observe a strong mutational strand bias, compatible with endogenous replication-coupled errors as the major source of mutations. Interestingly, while allelic ratios in general were consistent in RNA compared to DNA, some mutations in tRNAs displayed strong allelic imbalances caused by accumulation of unprocessed tRNA precursors. The effect was explained by altered secondary structure, demonstrating that correct tRNA folding is a major determinant for processing of polycistronic mitochondrial transcripts. Additionally, the data suggest that tRNA clusters are preferably processed in the 3' to 5' direction. Our study gives insights into mtDNA function in cancer and answers questions regarding mitochondrial tRNA biogenesis that are difficult to address in controlled experimental systems.

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DO - 10.1371/journal.pgen.1005333

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JO - P L o S Genetics

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Simultaneous DNA and RNA mapping of somatic mitochondrial mutations across diverse human cancers

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