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Methylation marks in blood DNA reveal breast cancer risk in patients fulfilling hereditary disease criteria.
Ruiz-De La Cruz, Miguel; Martínez-Gregorio, Héctor; Estela Díaz-Velásquez, Clara; Ambriz-Barrera, Fernando; Resendiz-Flores, Norma Gabriela; Gitler-Weingarten, Rina; Rojo-Castillo, María Patricia; Pradda, Didier; Oliver, Javier; Perdomo, Sandra; Gómez-García, Eva María; De La Cruz-Montoya, Aldo Hugo; Terrazas, Luis Ignacio; Torres-Mejía, Gabriela; Hernández-Hernández, Fidel de la Cruz; Vaca-Paniagua, Felipe.
Affiliation
  • Ruiz-De La Cruz M; Laboratorio Nacional en Salud, Diagnóstico Molecular y Efecto Ambiental en Enfermedades Crónico-Degenerativas, Facultad de Estudios Superiores Iztacala, Tlalnepantla, 54090, Mexico.
  • Martínez-Gregorio H; Unidad de Biomedicina, Facultad de Estudios Superiores Iztacala, UNAM, Tlalnepantla, 54090, Mexico.
  • Estela Díaz-Velásquez C; Centro de Investigación y de Estudios Avanzados IPN (CINVESTAV). Avenida Instituto Politécnico Nacional #2508, Colonia San Pedro Zacatenco, Delegación Gustavo A. Madero, Departamento de Infectómica y Patogénesis Molecular, Ciudad de México, Mexico.
  • Ambriz-Barrera F; Laboratorio Nacional en Salud, Diagnóstico Molecular y Efecto Ambiental en Enfermedades Crónico-Degenerativas, Facultad de Estudios Superiores Iztacala, Tlalnepantla, 54090, Mexico.
  • Resendiz-Flores NG; Unidad de Biomedicina, Facultad de Estudios Superiores Iztacala, UNAM, Tlalnepantla, 54090, Mexico.
  • Gitler-Weingarten R; Laboratorio Nacional en Salud, Diagnóstico Molecular y Efecto Ambiental en Enfermedades Crónico-Degenerativas, Facultad de Estudios Superiores Iztacala, Tlalnepantla, 54090, Mexico.
  • Rojo-Castillo MP; Laboratorio Nacional en Salud, Diagnóstico Molecular y Efecto Ambiental en Enfermedades Crónico-Degenerativas, Facultad de Estudios Superiores Iztacala, Tlalnepantla, 54090, Mexico.
  • Pradda D; Unidad de Biomedicina, Facultad de Estudios Superiores Iztacala, UNAM, Tlalnepantla, 54090, Mexico.
  • Oliver J; Laboratorio Nacional en Salud, Diagnóstico Molecular y Efecto Ambiental en Enfermedades Crónico-Degenerativas, Facultad de Estudios Superiores Iztacala, Tlalnepantla, 54090, Mexico.
  • Perdomo S; Unidad de Biomedicina, Facultad de Estudios Superiores Iztacala, UNAM, Tlalnepantla, 54090, Mexico.
  • Gómez-García EM; Fundación Alma I.A.P., 11560, Ciudad de México, México.
  • De La Cruz-Montoya AH; Instituto Nacional de Rehabilitación, Chorrillos, Peru.
  • Terrazas LI; Institute for Health Equity Research, Department of Health Science and Policy and Department of Environmental Medicine and Public Health at the Icahn School of Medicine at Mount Sinai, New York, NY, USA.
  • Torres-Mejía G; Medical Oncology Service, Hospitales Universitarios Regional y Virgen de la Victoria, Institute of Biomedical Research in Malaga, CIMES, University of Málaga, 29010, Málaga, Spain.
  • Hernández-Hernández FC; Genomic Epidemiology Branch, International Agency for Research on Cancer (IARC/WHO), 150 Cours Albert Thomas, 69372, Lyon, France.
  • Vaca-Paniagua F; Centro de Tratamiento de Cancer Metepec, Toluca, 50180, Mexico.
NPJ Precis Oncol ; 8(1): 136, 2024 Jun 19.
Article in En | MEDLINE | ID: mdl-38898118
ABSTRACT
Less than 15-20% of patients who meet the criteria for hereditary breast and ovarian cancer (HBOC) carry pathogenic coding genetic mutations, implying that other molecular mechanisms may contribute to the increased risk of this condition. DNA methylation in peripheral blood has been suggested as a potential epigenetic marker for the risk of breast cancer (BC). We aimed to discover methylation marks in peripheral blood associated with BC in 231 pre-treatment BC patients meeting HBOC criteria, testing negative for coding pathogenic variants, and 156 healthy controls, through methylation analysis by targeted bisulfite sequencing on 18 tumor suppressor gene promoters (330 CpG sites). We found i) hypermethylation in EPCAM (17 CpG sites; p = 0.017) and RAD51C (27 CpG sites; p = 0.048); ii) hypermethylation in 36 CpG-specific sites (FDR q < 0.05) in the BC patients; iii) four specific CpG sites were associated with a higher risk of BC (FDR q < 0.01, Bonferroni p < 0.001) cg89786999-FANCI (OR = 1.65; 95% CI1.2-2.2), cg23652916-PALB2 (OR = 2.83; 95% CI1.7-4.7), cg47630224-MSH2 (OR = 4.17; 95% CI2.1-8.5), and cg47596828-EPCAM (OR = 1.84; 95% CI1.5-2.3). Validation of cg47630224-MSH2 methylation in one Australian cohort showed an association with 3-fold increased BC risk (AUC 0.929; 95% CI 0.904-0.955). Our findings suggest that four DNA methylation CpG sites may be associated with a higher risk of BC, potentially serving as biomarkers in patients without detectable coding mutations.
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Full text: 1 Database: MEDLINE Language: En Journal: NPJ Precis Oncol Year: 2024 Type: Article Affiliation country: Mexico
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Full text: 1 Database: MEDLINE Language: En Journal: NPJ Precis Oncol Year: 2024 Type: Article Affiliation country: Mexico