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author Cagan, Alex
Baez-Ortega, Adrian
Brzozowska, Natalia
Abascal, Federico
Coorens, Tim H. H.
Sanders, Mathijs A.
Lawson, Andrew R. J.
Harvey, Luke M. R.
Bhosle, Shriram
Jones, David
Alcantara, Raul E.
Butler, Timothy M.
Hooks, Yvette
Roberts, Kirsty
Anderson, Elizabeth
Lunn, Sharna
Flach, Edmund
Spiro, Simon
Januszczak, Inez
Wrigglesworth, Ethan
Jenkins, Hannah
Dallas, Tilly
Masters, Nic
Perkins, Matthew W.
Deaville, Robert
Druce, Megan
Bogeska, Ruzhica
Milsom, Michael D.
Neumann, Björn
Gorman, Frank
Constantino-Casas, Fernando
Peachey, Laura
Bochynska, Diana
Smith, Ewan St. John
Gerstung, Moritz
Campbell, Peter J.
Murchison, Elizabeth P.
Stratton, Michael R.
Martincorena, Iñigo
author_facet Cagan, Alex
Baez-Ortega, Adrian
Brzozowska, Natalia
Abascal, Federico
Coorens, Tim H. H.
Sanders, Mathijs A.
Lawson, Andrew R. J.
Harvey, Luke M. R.
Bhosle, Shriram
Jones, David
Alcantara, Raul E.
Butler, Timothy M.
Hooks, Yvette
Roberts, Kirsty
Anderson, Elizabeth
Lunn, Sharna
Flach, Edmund
Spiro, Simon
Januszczak, Inez
Wrigglesworth, Ethan
Jenkins, Hannah
Dallas, Tilly
Masters, Nic
Perkins, Matthew W.
Deaville, Robert
Druce, Megan
Bogeska, Ruzhica
Milsom, Michael D.
Neumann, Björn
Gorman, Frank
Constantino-Casas, Fernando
Peachey, Laura
Bochynska, Diana
Smith, Ewan St. John
Gerstung, Moritz
Campbell, Peter J.
Murchison, Elizabeth P.
Stratton, Michael R.
Martincorena, Iñigo
author_sort Cagan, Alex
collection PubMed
description The rates and patterns of somatic mutation in normal tissues are largely unknown outside of humans(1–7). Comparative analyses can shed light on the diversity of mutagenesis across species, and on long-standing hypotheses about the evolution of somatic mutation rates and their role in cancer and ageing. Here we performed whole-genome sequencing of 208 intestinal crypts from 56 individuals to study the landscape of somatic mutation across 16 mammalian species. We found that somatic mutagenesis was dominated by seemingly endogenous mutational processes in all species, including 5-methylcytosine deamination and oxidative damage. With some differences, mutational signatures in other species resembled those described in humans(8), although the relative contribution of each signature varied across species. Notably, the somatic mutation rate per year varied greatly across species and exhibited a strong inverse relationship with species lifespan, with no other life-history trait studied showing a comparable association. Despite widely different life histories among the species we examined—including variation of around 30-fold in lifespan and around 40,000-fold in body mass—the somatic mutation burden at the end of lifespan varied only by a factor of around 3. These data unveil common mutational processes across mammals, and suggest that somatic mutation rates are evolutionarily constrained and may be a contributing factor in ageing.
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spelling pubmed-90210232022-04-29 Somatic mutation rates scale with lifespan across mammals Cagan, Alex Baez-Ortega, Adrian Brzozowska, Natalia Abascal, Federico Coorens, Tim H. H. Sanders, Mathijs A. Lawson, Andrew R. J. Harvey, Luke M. R. Bhosle, Shriram Jones, David Alcantara, Raul E. Butler, Timothy M. Hooks, Yvette Roberts, Kirsty Anderson, Elizabeth Lunn, Sharna Flach, Edmund Spiro, Simon Januszczak, Inez Wrigglesworth, Ethan Jenkins, Hannah Dallas, Tilly Masters, Nic Perkins, Matthew W. Deaville, Robert Druce, Megan Bogeska, Ruzhica Milsom, Michael D. Neumann, Björn Gorman, Frank Constantino-Casas, Fernando Peachey, Laura Bochynska, Diana Smith, Ewan St. John Gerstung, Moritz Campbell, Peter J. Murchison, Elizabeth P. Stratton, Michael R. Martincorena, Iñigo Nature Article The rates and patterns of somatic mutation in normal tissues are largely unknown outside of humans(1–7). Comparative analyses can shed light on the diversity of mutagenesis across species, and on long-standing hypotheses about the evolution of somatic mutation rates and their role in cancer and ageing. Here we performed whole-genome sequencing of 208 intestinal crypts from 56 individuals to study the landscape of somatic mutation across 16 mammalian species. We found that somatic mutagenesis was dominated by seemingly endogenous mutational processes in all species, including 5-methylcytosine deamination and oxidative damage. With some differences, mutational signatures in other species resembled those described in humans(8), although the relative contribution of each signature varied across species. Notably, the somatic mutation rate per year varied greatly across species and exhibited a strong inverse relationship with species lifespan, with no other life-history trait studied showing a comparable association. Despite widely different life histories among the species we examined—including variation of around 30-fold in lifespan and around 40,000-fold in body mass—the somatic mutation burden at the end of lifespan varied only by a factor of around 3. These data unveil common mutational processes across mammals, and suggest that somatic mutation rates are evolutionarily constrained and may be a contributing factor in ageing. Nature Publishing Group UK 2022-04-13 2022 /pmc/articles/PMC9021023/ /pubmed/35418684 http://dx.doi.org/10.1038/s41586-022-04618-z Text en © The Author(s) 2022 https://creativecommons.org/licenses/by/4.0/Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Article
Cagan, Alex
Baez-Ortega, Adrian
Brzozowska, Natalia
Abascal, Federico
Coorens, Tim H. H.
Sanders, Mathijs A.
Lawson, Andrew R. J.
Harvey, Luke M. R.
Bhosle, Shriram
Jones, David
Alcantara, Raul E.
Butler, Timothy M.
Hooks, Yvette
Roberts, Kirsty
Anderson, Elizabeth
Lunn, Sharna
Flach, Edmund
Spiro, Simon
Januszczak, Inez
Wrigglesworth, Ethan
Jenkins, Hannah
Dallas, Tilly
Masters, Nic
Perkins, Matthew W.
Deaville, Robert
Druce, Megan
Bogeska, Ruzhica
Milsom, Michael D.
Neumann, Björn
Gorman, Frank
Constantino-Casas, Fernando
Peachey, Laura
Bochynska, Diana
Smith, Ewan St. John
Gerstung, Moritz
Campbell, Peter J.
Murchison, Elizabeth P.
Stratton, Michael R.
Martincorena, Iñigo
Somatic mutation rates scale with lifespan across mammals
title Somatic mutation rates scale with lifespan across mammals
title_full Somatic mutation rates scale with lifespan across mammals
title_fullStr Somatic mutation rates scale with lifespan across mammals
title_full_unstemmed Somatic mutation rates scale with lifespan across mammals
title_short Somatic mutation rates scale with lifespan across mammals
title_sort somatic mutation rates scale with lifespan across mammals
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9021023/
https://www.ncbi.nlm.nih.gov/pubmed/35418684
http://dx.doi.org/10.1038/s41586-022-04618-z
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