Somatic mutations in the DNA repairome in prostate cancers in African Americans and Caucasians

Most hereditary tumors show aberrations in DNA repair genes or their regulators. In contrast, only a minority of sporadic tumors show alterations in these genes. As a result, genomic instability is currently considered an enhancer of tumorigenesis rather than an obligatory event in this process. How...

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Autores principales: Yadav, Santosh, Anbalagan, Muralidharan, Baddoo, Melody, Chellamuthu, Vinodh K., Mukhopadhyay, Sudurika, Woods, Carol, Jiang, Wei, Moroz, Krzysztof, Flemington, Erik K, Makridakis, Nick
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group UK 2020
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7239769/
https://www.ncbi.nlm.nih.gov/pubmed/32300177
http://dx.doi.org/10.1038/s41388-020-1280-x
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author Yadav, Santosh
Anbalagan, Muralidharan
Baddoo, Melody
Chellamuthu, Vinodh K.
Mukhopadhyay, Sudurika
Woods, Carol
Jiang, Wei
Moroz, Krzysztof
Flemington, Erik K
Makridakis, Nick
author_facet Yadav, Santosh
Anbalagan, Muralidharan
Baddoo, Melody
Chellamuthu, Vinodh K.
Mukhopadhyay, Sudurika
Woods, Carol
Jiang, Wei
Moroz, Krzysztof
Flemington, Erik K
Makridakis, Nick
author_sort Yadav, Santosh
collection PubMed
description Most hereditary tumors show aberrations in DNA repair genes or their regulators. In contrast, only a minority of sporadic tumors show alterations in these genes. As a result, genomic instability is currently considered an enhancer of tumorigenesis rather than an obligatory event in this process. However, tumor heterogeneity presents a significant technical challenge for most cancer genomics studies performed at less than 100× mean resolution depth. To address the importance of genomic instability in prostate carcinogenesis and tumor progression, we performed ultrahigh depth exome sequencing of 124 DNA damage repair/response (repairome) genes in 63 tumors and matched normal tissue samples in African Americans and Caucasians. The average sequence depth was 712-fold for DNA isolated from normal tissue and 368-fold for FFPE tumors. We identified 671 somatic mutations in tumors from African Americans and 762 somatic mutations in tumors in Caucasians. The most frequently mutated DNA repairome genes were EXO1, ATR, POLQ, NEIL3, ERCC6, BRCA2, BRCA1, XPC, JAG1, RPA1, POLE, ATM, and LIG1 in African American men, and POLQ, NEIL3, POLB, BRCA2, EXO1, ERCC6, ATR, RBBP8, BRCA1, ATM, JAG1, XPC, and POLE in Caucasians. We found that 89% of tumors had at least one mutation in nucleotide excision repair pathway genes in African Americans, whereas >40% of tumors had mutations in base excision repair pathway genes in Caucasians. We further identified a marginal increase in mutation rate in tumors in African Americans with increasing age. Tumors in Caucasians did not show a correlation with age, but a progressive increase in the mutation rate was observed at higher Gleason scores. Our data reveal significant differences in the molecular signatures in the DNA repairome in prostate cancer between African Americans and Caucasians. These data also have substantial implications regarding the well-known health disparities in prostate cancer, such as the higher mortality in African Americans than Caucasians.
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spelling pubmed-72397692020-05-29 Somatic mutations in the DNA repairome in prostate cancers in African Americans and Caucasians Yadav, Santosh Anbalagan, Muralidharan Baddoo, Melody Chellamuthu, Vinodh K. Mukhopadhyay, Sudurika Woods, Carol Jiang, Wei Moroz, Krzysztof Flemington, Erik K Makridakis, Nick Oncogene Article Most hereditary tumors show aberrations in DNA repair genes or their regulators. In contrast, only a minority of sporadic tumors show alterations in these genes. As a result, genomic instability is currently considered an enhancer of tumorigenesis rather than an obligatory event in this process. However, tumor heterogeneity presents a significant technical challenge for most cancer genomics studies performed at less than 100× mean resolution depth. To address the importance of genomic instability in prostate carcinogenesis and tumor progression, we performed ultrahigh depth exome sequencing of 124 DNA damage repair/response (repairome) genes in 63 tumors and matched normal tissue samples in African Americans and Caucasians. The average sequence depth was 712-fold for DNA isolated from normal tissue and 368-fold for FFPE tumors. We identified 671 somatic mutations in tumors from African Americans and 762 somatic mutations in tumors in Caucasians. The most frequently mutated DNA repairome genes were EXO1, ATR, POLQ, NEIL3, ERCC6, BRCA2, BRCA1, XPC, JAG1, RPA1, POLE, ATM, and LIG1 in African American men, and POLQ, NEIL3, POLB, BRCA2, EXO1, ERCC6, ATR, RBBP8, BRCA1, ATM, JAG1, XPC, and POLE in Caucasians. We found that 89% of tumors had at least one mutation in nucleotide excision repair pathway genes in African Americans, whereas >40% of tumors had mutations in base excision repair pathway genes in Caucasians. We further identified a marginal increase in mutation rate in tumors in African Americans with increasing age. Tumors in Caucasians did not show a correlation with age, but a progressive increase in the mutation rate was observed at higher Gleason scores. Our data reveal significant differences in the molecular signatures in the DNA repairome in prostate cancer between African Americans and Caucasians. These data also have substantial implications regarding the well-known health disparities in prostate cancer, such as the higher mortality in African Americans than Caucasians. Nature Publishing Group UK 2020-04-16 2020 /pmc/articles/PMC7239769/ /pubmed/32300177 http://dx.doi.org/10.1038/s41388-020-1280-x Text en © The Author(s), under exclusive licence to Springer Nature Limited 2020 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/.
spellingShingle Article
Yadav, Santosh
Anbalagan, Muralidharan
Baddoo, Melody
Chellamuthu, Vinodh K.
Mukhopadhyay, Sudurika
Woods, Carol
Jiang, Wei
Moroz, Krzysztof
Flemington, Erik K
Makridakis, Nick
Somatic mutations in the DNA repairome in prostate cancers in African Americans and Caucasians
title Somatic mutations in the DNA repairome in prostate cancers in African Americans and Caucasians
title_full Somatic mutations in the DNA repairome in prostate cancers in African Americans and Caucasians
title_fullStr Somatic mutations in the DNA repairome in prostate cancers in African Americans and Caucasians
title_full_unstemmed Somatic mutations in the DNA repairome in prostate cancers in African Americans and Caucasians
title_short Somatic mutations in the DNA repairome in prostate cancers in African Americans and Caucasians
title_sort somatic mutations in the dna repairome in prostate cancers in african americans and caucasians
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7239769/
https://www.ncbi.nlm.nih.gov/pubmed/32300177
http://dx.doi.org/10.1038/s41388-020-1280-x
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