Exome sequencing identified rare recurrent copy number variants and hereditary breast cancer susceptibility

Copy number variants (CNVs) are a major source of genetic variation and can disrupt genes or affect gene dosage. They are known to be causal or underlie predisposition to various diseases. However, the role of CNVs in inherited breast cancer susceptibility has not been thoroughly investigated. To ad...

Descripción completa

Detalles Bibliográficos
Autores principales: Kumpula, Timo A., Vorimo, Sandra, Mattila, Taneli T., O’Gorman, Luke, Astuti, Galuh, Tervasmäki, Anna, Koivuluoma, Susanna, Mattila, Tiina M., Grip, Mervi, Winqvist, Robert, Kuismin, Outi, Moilanen, Jukka, Hoischen, Alexander, Gilissen, Christian, Mantere, Tuomo, Pylkäs, Katri
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10449128/
https://www.ncbi.nlm.nih.gov/pubmed/37578974
http://dx.doi.org/10.1371/journal.pgen.1010889
_version_ 1785094878359715840
author Kumpula, Timo A.
Vorimo, Sandra
Mattila, Taneli T.
O’Gorman, Luke
Astuti, Galuh
Tervasmäki, Anna
Koivuluoma, Susanna
Mattila, Tiina M.
Grip, Mervi
Winqvist, Robert
Kuismin, Outi
Moilanen, Jukka
Hoischen, Alexander
Gilissen, Christian
Mantere, Tuomo
Pylkäs, Katri
author_facet Kumpula, Timo A.
Vorimo, Sandra
Mattila, Taneli T.
O’Gorman, Luke
Astuti, Galuh
Tervasmäki, Anna
Koivuluoma, Susanna
Mattila, Tiina M.
Grip, Mervi
Winqvist, Robert
Kuismin, Outi
Moilanen, Jukka
Hoischen, Alexander
Gilissen, Christian
Mantere, Tuomo
Pylkäs, Katri
author_sort Kumpula, Timo A.
collection PubMed
description Copy number variants (CNVs) are a major source of genetic variation and can disrupt genes or affect gene dosage. They are known to be causal or underlie predisposition to various diseases. However, the role of CNVs in inherited breast cancer susceptibility has not been thoroughly investigated. To address this, we performed whole-exome sequencing based analysis of rare CNVs in 98 high-risk Northern Finnish breast cancer cases. After filtering, selected candidate alleles were validated and characterized with a combination of orthogonal methods, including PCR-based approaches, optical genome mapping and long-read sequencing. This revealed three recurrent alterations: a 31 kb deletion co-occurring with a retrotransposon insertion (delins) in RAD52, a 13.4 kb deletion in HSD17B14 and a 64 kb partial duplication of RAD51C. Notably, all these genes encode proteins involved in pathways previously identified as essential for breast cancer development. Variants were genotyped in geographically matched cases and controls (altogether 278 hereditary and 1983 unselected breast cancer cases, and 1229 controls). The RAD52 delins and HSD17B14 deletion both showed significant enrichment among cases with indications of hereditary disease susceptibility. RAD52 delins was identified in 7/278 cases (2.5%, P = 0.034, OR = 2.86, 95% CI = 1.10–7.45) and HSD17B14 deletion in 8/278 cases (2.9%, P = 0.014, OR = 3.28, 95% CI = 1.31–8.23), the frequency of both variants in the controls being 11/1229 (0.9%). This suggests a role for RAD52 and HSD17B14 in hereditary breast cancer susceptibility. The RAD51C duplication was very rare, identified only in 2/278 of hereditary cases and 2/1229 controls (P = 0.157, OR = 4.45, 95% CI = 0.62–31.70). The identification of recurrent CNVs in these genes, and especially the relatively high frequency of RAD52 and HSD17B14 alterations in the Finnish population, highlights the importance of studying CNVs alongside single nucleotide variants when searching for genetic factors underlying hereditary disease predisposition.
format Online
Article
Text
id pubmed-10449128
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-104491282023-08-25 Exome sequencing identified rare recurrent copy number variants and hereditary breast cancer susceptibility Kumpula, Timo A. Vorimo, Sandra Mattila, Taneli T. O’Gorman, Luke Astuti, Galuh Tervasmäki, Anna Koivuluoma, Susanna Mattila, Tiina M. Grip, Mervi Winqvist, Robert Kuismin, Outi Moilanen, Jukka Hoischen, Alexander Gilissen, Christian Mantere, Tuomo Pylkäs, Katri PLoS Genet Research Article Copy number variants (CNVs) are a major source of genetic variation and can disrupt genes or affect gene dosage. They are known to be causal or underlie predisposition to various diseases. However, the role of CNVs in inherited breast cancer susceptibility has not been thoroughly investigated. To address this, we performed whole-exome sequencing based analysis of rare CNVs in 98 high-risk Northern Finnish breast cancer cases. After filtering, selected candidate alleles were validated and characterized with a combination of orthogonal methods, including PCR-based approaches, optical genome mapping and long-read sequencing. This revealed three recurrent alterations: a 31 kb deletion co-occurring with a retrotransposon insertion (delins) in RAD52, a 13.4 kb deletion in HSD17B14 and a 64 kb partial duplication of RAD51C. Notably, all these genes encode proteins involved in pathways previously identified as essential for breast cancer development. Variants were genotyped in geographically matched cases and controls (altogether 278 hereditary and 1983 unselected breast cancer cases, and 1229 controls). The RAD52 delins and HSD17B14 deletion both showed significant enrichment among cases with indications of hereditary disease susceptibility. RAD52 delins was identified in 7/278 cases (2.5%, P = 0.034, OR = 2.86, 95% CI = 1.10–7.45) and HSD17B14 deletion in 8/278 cases (2.9%, P = 0.014, OR = 3.28, 95% CI = 1.31–8.23), the frequency of both variants in the controls being 11/1229 (0.9%). This suggests a role for RAD52 and HSD17B14 in hereditary breast cancer susceptibility. The RAD51C duplication was very rare, identified only in 2/278 of hereditary cases and 2/1229 controls (P = 0.157, OR = 4.45, 95% CI = 0.62–31.70). The identification of recurrent CNVs in these genes, and especially the relatively high frequency of RAD52 and HSD17B14 alterations in the Finnish population, highlights the importance of studying CNVs alongside single nucleotide variants when searching for genetic factors underlying hereditary disease predisposition. Public Library of Science 2023-08-14 /pmc/articles/PMC10449128/ /pubmed/37578974 http://dx.doi.org/10.1371/journal.pgen.1010889 Text en © 2023 Kumpula et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Kumpula, Timo A.
Vorimo, Sandra
Mattila, Taneli T.
O’Gorman, Luke
Astuti, Galuh
Tervasmäki, Anna
Koivuluoma, Susanna
Mattila, Tiina M.
Grip, Mervi
Winqvist, Robert
Kuismin, Outi
Moilanen, Jukka
Hoischen, Alexander
Gilissen, Christian
Mantere, Tuomo
Pylkäs, Katri
Exome sequencing identified rare recurrent copy number variants and hereditary breast cancer susceptibility
title Exome sequencing identified rare recurrent copy number variants and hereditary breast cancer susceptibility
title_full Exome sequencing identified rare recurrent copy number variants and hereditary breast cancer susceptibility
title_fullStr Exome sequencing identified rare recurrent copy number variants and hereditary breast cancer susceptibility
title_full_unstemmed Exome sequencing identified rare recurrent copy number variants and hereditary breast cancer susceptibility
title_short Exome sequencing identified rare recurrent copy number variants and hereditary breast cancer susceptibility
title_sort exome sequencing identified rare recurrent copy number variants and hereditary breast cancer susceptibility
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10449128/
https://www.ncbi.nlm.nih.gov/pubmed/37578974
http://dx.doi.org/10.1371/journal.pgen.1010889
work_keys_str_mv AT kumpulatimoa exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility
AT vorimosandra exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility
AT mattilatanelit exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility
AT ogormanluke exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility
AT astutigaluh exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility
AT tervasmakianna exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility
AT koivuluomasusanna exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility
AT mattilatiinam exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility
AT gripmervi exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility
AT winqvistrobert exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility
AT kuisminouti exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility
AT moilanenjukka exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility
AT hoischenalexander exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility
AT gilissenchristian exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility
AT manteretuomo exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility
AT pylkaskatri exomesequencingidentifiedrarerecurrentcopynumbervariantsandhereditarybreastcancersusceptibility

Ejemplares similares