| Literature DB >> 33287145 |
Maria Teresa Vietri1,2, Gemma Caliendo2, Giovanna D'Elia2, Marianna Resse1,2, Amelia Casamassimi1, Pellegrino Biagio Minucci1,2, Concetta Dello Ioio3, Michele Cioffi1,2, Anna Maria Molinari1,2.
Abstract
Double heterozygosity (DH) in BRCA1 and BRCA2 genes and double mutation (DM) in BRCA1 or BRCA2 are extremely rare events in the general population, and few cases have been reported worldwide so far. Here, we describe five probands, all women, with breast and/or ovarian cancer and their families. Particularly, we identified two probands with DH in the BRCA1/2 genes with a frequency of 0.3% and three probands with DM in the BRCA2 gene with a frequency of 0.5%. The DH BRCA1 c.547+2T>A (IVS8+2T>A)/BRCA2 c.2830A>T (p.Lys944Ter) and BRCA1 c.3752_3755GTCT (p.Ser1253fs)/BRCA2 c.425+2T>C (IVS4+2T>C) have not been described together so far. The DM in BRCA2, c.631G>A (p.Val211Ile) and c.7008-2A>T (IVS13-2A>T), found in three unrelated probands, was previously reported in further unrelated patients. Due to its peculiarity, it is likely that both pathogenic variants descend from a common ancestor and, therefore, are founder mutations. Interestingly, analyzing the tumor types occurring in DH and DM families, we observed ovarian cancer only in DH families, probably due to the presence in DH patients of BRCA1 pathogenic variants, which predispose one more to ovarian cancer onset. Furthermore, male breast cancer and pancreatic cancer ensued in families with DM but not with DH. These data confirm that BRCA2 pathogenic variants have greater penetrance to develop breast cancer in men and are associated with an increased risk of pancreatic cancer.Entities:
Keywords: BRCA1; BRCA2; double heterozygosity (DH); double mutations (DM); hereditary breast and ovarian cancer
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Year: 2020 PMID: 33287145 PMCID: PMC7761639 DOI: 10.3390/genes11121451
Source DB: PubMed Journal: Genes (Basel) ISSN: 2073-4425 Impact factor: 4.096