Evaluation of the contribution of germline variants in BRCA1 and BRCA2 to uveal and cutaneous melanoma.

Alleles Australia BRCA1 Protein / genetics BRCA2 Protein / genetics Computational Biology Denmark Exome Female Frameshift Mutation Gene Deletion Gene Frequency Genetic Predisposition to Disease Germ-Line Mutation Humans Male Melanoma / genetics Netherlands Skin Neoplasms / genetics Sweden Uveal Neoplasms / genetics Whole Genome Sequencing Melanoma, Cutaneous Malignant

Journal

Melanoma research

ISSN: 1473-5636

Titre abrégé: Melanoma Res

Pays: England

ID NLM: 9109623

Informations de publication

Date de publication:
10 2019

Historique:

entrez: 30 8 2019

pubmed: 30 8 2019

medline: 9 7 2020

Statut: ppublish

Résumé

Germline mutations of BRCA1 and BRCA2 predispose individuals to a high risk of breast and ovarian cancer, and elevated risk of other cancers, including those of the pancreas and prostate. BRCA2 mutation carriers may have increased risk of uveal melanoma (UM) and cutaneous melanoma (CM), but associations with these cancers in BRCA1 mutation carriers have been mixed. Here, we further assessed whether UM and CM are associated with BRCA1 or BRCA2 by assessing the presence, segregation and reported/predicted pathogenicity of rare germline mutations (variant allele frequency < 0.01) in families with multiple members affected by these cancers. Whole-genome or exome sequencing was performed on 160 CM and/or UM families from Australia, the Netherlands, Denmark and Sweden. Between one and five cases were sequenced from each family, totalling 307 individuals. Sanger sequencing was performed to validate BRCA1 and BRCA2 germline variants and to assess carrier status in other available family members. A nonsense and a frameshift mutation were identified in BRCA1, both resulting in premature truncation of the protein (the first at p.Q516 and the second at codon 91, after the introduction of seven amino acids due to a frameshift deletion). These variants co-segregated with CM in individuals who consented for testing and were present in individuals with pancreatic, prostate and breast cancer in the respective families. In addition, 33 rare missense mutations (variant allele frequency ranging from 0.00782 to 0.000001 in the aggregated ExAC data) were identified in 34 families. Examining the previously reported evidence of functional consequence of these variants revealed all had been classified as either benign or of unknown consequence. Seeking further evidence of an association between BRCA1 variants and melanoma, we examined two whole-genome/exome sequenced collections of sporadic CM patients (total N = 763). We identified one individual with a deleterious BRCA1 variant, however, this allele was lost (with the wild-type allele remaining) in the corresponding CM, indicating that defective BRCA1 was not a driver of tumorigenesis in this instance. Although this is the first time that deleterious BRCA1 mutations have been described in high-density CM families, we conclude that there is an insufficient burden of evidence to state that the increased familial CM or UM susceptibility is because of these variants. In addition, in conjunction with other studies, we conclude that the previously described association between BRCA2 mutations and UM susceptibility represents a rare source of increased risk.

Identifiants

DOI: 10.1097/CMR.0000000000000613 PMID: 31464824 PMC: PMC6716616

pubmed: 31464824

doi: 10.1097/CMR.0000000000000613

pii: 00008390-201910000-00004

pmc: PMC6716616

mid: NIHMS1525431

doi:

Substances chimiques

BRCA1 Protein 0

BRCA1 protein, human 0

BRCA2 Protein 0

BRCA2 protein, human 0

Types de publication

Journal Article Research Support, Non-U.S. Gov't

Langues

eng

Sous-ensembles de citation

Pagination

483-490

Subventions

Organisme : NCI NIH HHS

ID : R01 CA088363

Pays : United States

Organisme : Intramural NIH HHS

ID : Z99 CA999999

Pays : United States

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