PLoS ONE (Jan 2019)

Mexican BRCA1 founder mutation: Shortening the gap in genetic assessment for hereditary breast and ovarian cancer patients.

  • Veronica Fragoso-Ontiveros,
  • Jose Antonio Velázquez-Aragón,
  • Paulina Maria Nuñez-Martínez,
  • Maria de la Luz Mejía-Aguayo,
  • Silvia Vidal-Millán,
  • Abraham Pedroza-Torres,
  • Yuliana Sánchez-Contreras,
  • Miguel Angel Ramírez-Otero,
  • Rodolfo Muñiz-Mendoza,
  • Julieta Domínguez-Ortíz,
  • Talia Wegman-Ostrosky,
  • Juan Enrique Bargalló-Rocha,
  • Dolores Gallardo-Rincón,
  • Nancy Reynoso-Noveron,
  • Cristian Arriaga-Canon,
  • Abelardo Meneses-García,
  • Luis Alonso Herrera-Montalvo,
  • Rosa Maria Alvarez-Gomez

DOI
https://doi.org/10.1371/journal.pone.0222709
Journal volume & issue
Vol. 14, no. 9
p. e0222709

Abstract

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The deletion of exons 9 to 12 of BRCA1 (9-12 del BRCA1) is considered a founder mutation in the Mexican population. We evaluate the usefulness of the target detection of 9-12 del BRCA1 as the first molecular diagnostic strategy in patients with Hereditary Breast and Ovarian Cancer (HBOC). We performed the genetic assessment of 637 patients with suspected HBOC. The region corresponding to the breakpoints for the 9-12 del BRCA1 was amplified by polymerase chain reaction (PCR). An analysis of the clinical data of the carriers and non-carriers was done, searching for characteristics that correlated with the deletion. The 9-12 del BRCA1 was detected in 5% of patients with suspected HBOC (30/637). In patients diagnosed with ovarian cancer, 13 of 30 were 9-12 del BRCA1 carriers, which represents 43%. We found a significant association between the 9-12 del BRCA1 carriers with triple negative breast cancer and high-grade papillary serous ovarian cancer. We concluded that the detection of the 9-12 del BRCA1 is useful as a first molecular diagnostic strategy in the Mexican population. In particular, it shortens the gap in genetic assessment in patients with triple negative breast cancer and ovarian cancer.