Comprehensive analysis of mutational signatures reveals distinct patterns and molecular processes across 27 pediatric cancers

Venu Thatikonda; S. M.Ashiqul Islam; Robert J. Autry; Barbara C. Jones; Susanne N. Gröbner; Gregor Warsow; Barbara Hutter; Daniel Huebschmann; Stefan Fröhling; Marcel Kool; Mirjam Blattner-Johnson; David T.W. Jones; Ludmil B. Alexandrov; Stefan M. Pfister; Natalie Jäger

doi:10.1038/s43018-022-00509-4

Comprehensive analysis of mutational signatures reveals distinct patterns and molecular processes across 27 pediatric cancers

Venu Thatikonda
, S. M.Ashiqul Islam
, Robert J. Autry
, Barbara C. Jones
, Susanne N. Gröbner
, Gregor Warsow
, Barbara Hutter
, Daniel Huebschmann
, Stefan Fröhling
, Marcel Kool
, Mirjam Blattner-Johnson
, David T.W. Jones
, Ludmil B. Alexandrov
, Stefan M. Pfister (Corresponding Author)
, Natalie Jäger (Corresponding Author)

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

57 Citations (Scopus)

Abstract

Analysis of mutational signatures can reveal underlying molecular mechanisms of the processes that have imprinted the somatic mutations found in cancer genomes. Here, we analyze single base substitutions and small insertions and deletions in pediatric cancers encompassing 785 whole-genome sequenced tumors from 27 molecularly defined cancer subtypes. We identified only a small number of mutational signatures active in pediatric cancers, compared with previously analyzed adult cancers. Further, we report a significant difference in the proportion of pediatric tumors showing homologous recombination repair defect signatures compared with previous analyses. In pediatric leukemias, we identified an indel signature, not previously reported, characterized by long insertions in nonrepeat regions, affecting mainly intronic and intergenic regions, but also exons of known cancer genes. We provide a systematic overview of COSMIC v.3 mutational signatures active across pediatric cancers, which is highly relevant for understanding tumor biology and enabling future research in defining biomarkers of treatment response.

Original language	English
Pages (from-to)	276-289
Number of pages	14
Journal	Nature Cancer
Volume	4
Issue number	2
DOIs	https://doi.org/10.1038/s43018-022-00509-4
Publication status	Published - Feb 2023
Externally published	Yes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Field of Science*

3.2 Clinical medicine
3.1 Basic medicine

Publication Type*

1.1. Scientific article indexed in Web of Science and/or Scopus database

Access to Document

10.1038/s43018-022-00509-4Licence: CC BY

Cite this

Thatikonda, V., Islam, S. M. A., Autry, R. J., Jones, B. C., Gröbner, S. N., Warsow, G., Hutter, B., Huebschmann, D., Fröhling, S., Kool, M., Blattner-Johnson, M., Jones, D. T. W., Alexandrov, L. B., Pfister, S. M., & Jäger, N. (2023). Comprehensive analysis of mutational signatures reveals distinct patterns and molecular processes across 27 pediatric cancers. Nature Cancer, 4(2), 276-289. https://doi.org/10.1038/s43018-022-00509-4

@article{dc3f40d90c8c4bfabf0612c01fcb075f,

title = "Comprehensive analysis of mutational signatures reveals distinct patterns and molecular processes across 27 pediatric cancers",

abstract = "Analysis of mutational signatures can reveal underlying molecular mechanisms of the processes that have imprinted the somatic mutations found in cancer genomes. Here, we analyze single base substitutions and small insertions and deletions in pediatric cancers encompassing 785 whole-genome sequenced tumors from 27 molecularly defined cancer subtypes. We identified only a small number of mutational signatures active in pediatric cancers, compared with previously analyzed adult cancers. Further, we report a significant difference in the proportion of pediatric tumors showing homologous recombination repair defect signatures compared with previous analyses. In pediatric leukemias, we identified an indel signature, not previously reported, characterized by long insertions in nonrepeat regions, affecting mainly intronic and intergenic regions, but also exons of known cancer genes. We provide a systematic overview of COSMIC v.3 mutational signatures active across pediatric cancers, which is highly relevant for understanding tumor biology and enabling future research in defining biomarkers of treatment response.",

author = "Venu Thatikonda and Islam, \{S. M.Ashiqul\} and Autry, \{Robert J.\} and Jones, \{Barbara C.\} and Gr{\"o}bner, \{Susanne N.\} and Gregor Warsow and Barbara Hutter and Daniel Huebschmann and Stefan Fr{\"o}hling and Marcel Kool and Mirjam Blattner-Johnson and Jones, \{David T.W.\} and Alexandrov, \{Ludmil B.\} and Pfister, \{Stefan M.\} and Natalie J{\"a}ger",

note = "Publisher Copyright: {\textcopyright} 2023, The Author(s).",

year = "2023",

month = feb,

doi = "10.1038/s43018-022-00509-4",

language = "English",

volume = "4",

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journal = "Nature Cancer",

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Thatikonda, V, Islam, SMA, Autry, RJ, Jones, BC, Gröbner, SN, Warsow, G, Hutter, B, Huebschmann, D, Fröhling, S, Kool, M, Blattner-Johnson, M, Jones, DTW, Alexandrov, LB, Pfister, SM & Jäger, N 2023, 'Comprehensive analysis of mutational signatures reveals distinct patterns and molecular processes across 27 pediatric cancers', Nature Cancer, vol. 4, no. 2, pp. 276-289. https://doi.org/10.1038/s43018-022-00509-4

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AU - Thatikonda, Venu

AU - Islam, S. M.Ashiqul

AU - Autry, Robert J.

AU - Jones, Barbara C.

AU - Gröbner, Susanne N.

AU - Warsow, Gregor

AU - Hutter, Barbara

AU - Huebschmann, Daniel

AU - Fröhling, Stefan

AU - Kool, Marcel

AU - Blattner-Johnson, Mirjam

AU - Jones, David T.W.

AU - Alexandrov, Ludmil B.

AU - Pfister, Stefan M.

AU - Jäger, Natalie

PY - 2023/2

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N2 - Analysis of mutational signatures can reveal underlying molecular mechanisms of the processes that have imprinted the somatic mutations found in cancer genomes. Here, we analyze single base substitutions and small insertions and deletions in pediatric cancers encompassing 785 whole-genome sequenced tumors from 27 molecularly defined cancer subtypes. We identified only a small number of mutational signatures active in pediatric cancers, compared with previously analyzed adult cancers. Further, we report a significant difference in the proportion of pediatric tumors showing homologous recombination repair defect signatures compared with previous analyses. In pediatric leukemias, we identified an indel signature, not previously reported, characterized by long insertions in nonrepeat regions, affecting mainly intronic and intergenic regions, but also exons of known cancer genes. We provide a systematic overview of COSMIC v.3 mutational signatures active across pediatric cancers, which is highly relevant for understanding tumor biology and enabling future research in defining biomarkers of treatment response.

AB - Analysis of mutational signatures can reveal underlying molecular mechanisms of the processes that have imprinted the somatic mutations found in cancer genomes. Here, we analyze single base substitutions and small insertions and deletions in pediatric cancers encompassing 785 whole-genome sequenced tumors from 27 molecularly defined cancer subtypes. We identified only a small number of mutational signatures active in pediatric cancers, compared with previously analyzed adult cancers. Further, we report a significant difference in the proportion of pediatric tumors showing homologous recombination repair defect signatures compared with previous analyses. In pediatric leukemias, we identified an indel signature, not previously reported, characterized by long insertions in nonrepeat regions, affecting mainly intronic and intergenic regions, but also exons of known cancer genes. We provide a systematic overview of COSMIC v.3 mutational signatures active across pediatric cancers, which is highly relevant for understanding tumor biology and enabling future research in defining biomarkers of treatment response.

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AN - SCOPUS:85146840196

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JO - Nature Cancer

JF - Nature Cancer

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ER -

Comprehensive analysis of mutational signatures reveals distinct patterns and molecular processes across 27 pediatric cancers

Abstract

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