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Constitutional mosaicism for a BRCA2 mutation as a cause of early-onset breast cancer
Constitutional mosaicism for a BRCA2 mutation as a cause of early-onset breast cancer
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Constitutional mosaicism for a BRCA2 mutation as a cause of early-onset breast cancer
Constitutional mosaicism for a BRCA2 mutation as a cause of early-onset breast cancer

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Constitutional mosaicism for a BRCA2 mutation as a cause of early-onset breast cancer
Constitutional mosaicism for a BRCA2 mutation as a cause of early-onset breast cancer
Journal Article

Constitutional mosaicism for a BRCA2 mutation as a cause of early-onset breast cancer

2020
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Overview
Germline mutations in the BRCA1 and BRCA2 genes cause hereditary breast and ovarian cancer syndrome (HBOC). Mutations in these genes are usually inherited, and reports of de novo BRCA1/2 mutations are rare. To date, only one patient with low-level BRCA1 mutation mosaicism has been published. We report on a breast cancer patient with constitutional somatic mosaicism of a BRCA2 mutation. BRCA2 mutation c.9294C>G, p.(Tyr3098Ter) was detected in 20% of reads in DNA extracted from peripheral blood using next-generation sequencing (NGS). The BRCA2 mutation was subsequently observed at similar levels in normal breast tissue, adipose tissue, normal right fallopian tube tissue and ovaries of the patient, suggesting that this mutation occurred early in embryonic development. This is the first case to report constitutional mosaicism for a BRCA2 mutation and shows that BRCA2 mosaicism can underlie early-onset breast cancer. NGS for BRCA1/2 should be considered for patients whose tumors harbor a BRCA1/2 mutation and for individuals suggestive of genetic predisposition but without a family history of HBO.