Cancers (Jan 2022)

Beyond BRCA1/2: Homologous Recombination Repair Genetic Profile in a Large Cohort of Apulian Ovarian Cancers

  • Antonella Turchiano,
  • Daria Carmela Loconte,
  • Rosalba De Nola,
  • Francesca Arezzo,
  • Giulia Chiarello,
  • Antonino Pantaleo,
  • Matteo Iacoviello,
  • Rosanna Bagnulo,
  • Annunziata De Luisi,
  • Sonia Perrelli,
  • Stefania Martino,
  • Carlotta Ranieri,
  • Antonella Garganese,
  • Alessandro Stella,
  • Cinzia Forleo,
  • Vera Loizzi,
  • Marco Marinaccio,
  • Ettore Cicinelli,
  • Gennaro Cormio,
  • Nicoletta Resta

DOI
https://doi.org/10.3390/cancers14020365
Journal volume & issue
Vol. 14, no. 2
p. 365

Abstract

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Background: Pathogenic variants in homologous recombination repair (HRR) genes other than BRCA1/2 have been associated with a high risk of ovarian cancer (OC). In current clinical practice, genetic testing is generally limited to BRCA1/2. Herein, we investigated the mutational status of both BRCA1/2 and 5 HRR genes in 69 unselected OC, evaluating the advantage of multigene panel testing in everyday clinical practice. Methods: We analyzed 69 epithelial OC samples using an NGS custom multigene panel of the 5 HRR pathways genes, beyond the genetic screening routine of BRCA1/2 testing. Results: Overall, 19 pathogenic variants (27.5%) were detected. The majority (21.7%) of patients displayed a deleterious mutation in BRCA1/2, whereas 5.8% harbored a pathogenic variant in one of the HRR genes. Additionally, there were 14 (20.3%) uncertain significant variants (VUS). The assessment of germline mutational status showed that a small number of variants (five) were not detected in the corresponding blood sample. Notably, we detected one BRIP1 and four BRCA1/2 deleterious variants in the low-grade serous and endometrioid histology OC, respectively. Conclusion: We demonstrate that using a multigene panel beyond BRCA1/2 improves the diagnostic yield in OC testing, and it could produce clinically relevant results.

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