AI Article Synopsis

  • NCCN Guidelines suggest BRCA genetic testing is appropriate for individuals with over a 5% chance of being carriers, raising questions about the cost-effectiveness for those without a family history of tumors.
  • An analysis of 268 breast cancer patients found that triple-negative breast cancer (TNBC) patients diagnosed before age 60 had a 22.6% prevalence of BRCA mutations, with higher rates in younger age groups.
  • In contrast, luminal-like breast cancer patients showed a lower BRCA mutation rate (6.4%), indicating potential involvement of other genetic factors besides BRCA.

Article Abstract

NCCN Guidelines recommend BRCA genetic testing in individuals with a probability >5% of being a carrier. Nonetheless, the cost-effectiveness of testing individuals with no tumor family history is still debated, especially when BRCA testing is offered by the national health service. Our analysis evaluated the rate of BRCA pathogenic or likely-pathogenic variants in 159 triple-negative breast cancer (TNBC) patients diagnosed ≤60 years, and 109 luminal-like breast cancer (BC) patients diagnosed ≤35 without breast and/or ovarian family histories. In TNBC patients, BRCA mutation prevalence was 22.6% (21.4% BRCA1). Mutation prevalence was 64.2% ≤30 years, 31.8% in patients aged 31-40, 16.1% for those aged 41-50 and 7.9% in 51-60s. A total of 40% of patients with estrogen receptors (ER) 1-9% were BRCA1 carriers. BRCA detection rate in early-onset BCs was 6.4% (4.6% ). Mutation prevalence was 0% between 0-25 years, 9% between 26-30 years and 6% between 31-35 years. In conclusion, BRCA testing is recommended in TNBC patients diagnosed ≤60 years, regardless of family cancer history or histotype, and by using immunohistochemical staining <10% for both ER and/PR. In luminal-like early-onset BC, a lower BRCA detection rate was observed, suggesting a role for other predisposing genes along with BRCA genetic testing.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7281631PMC
http://dx.doi.org/10.3390/cancers12051252DOI Listing

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