Silencing of tumor suppressor genes RASSF1A, SLIT2, and WIF1 by promoter hypermethylation in hereditary breast cancer

Alvarez, Carolina; Tapia, Teresa; Cornejo, Valeria; Fernandez, Wanda; Muñoz, Alex; Camus, Mauricio; Alvarez, Manuel; Devoto, Luigi; Carvallo, Pilar

Artículo de revista

Fecha

2013

Registro en:

Molecular Carcinogenesis, Volumen 52, Issue 6, 2018, Pages 475-487

08991987

10982744

10.1002/mc.21881

https://repositorio.uchile.cl/handle/2250/165963

Autor

Alvarez, Carolina

Tapia, Teresa

Cornejo, Valeria

Fernandez, Wanda

Muñoz, Alex

Camus, Mauricio

Alvarez, Manuel

Devoto, Luigi

Carvallo, Pilar

Institución

Universidad de Chile

Resumen

Promoter hypermethylation is gaining strength as one of the main mechanisms through which tumor suppressor genes are silenced during tumor progression. Three tumor suppressor genes are frequently found methylated in their promoter, in concordance with absence of expression, RASSF1A, SLIT2, and WIF1. In addition, a previous array-CGH analysis from our group showed that these genes are found in deleted genomic regions observed in hereditary breast cancer tumors. In the present work we analyzed the methylation status of these three tumor suppressor gene promoters in 47 hereditary breast cancer tumors. Promoter methylation status analysis of hereditary breast tumors revealed high methylation frequencies for the three genes (67% RASSF1A, 80% SLIT2, and 72% WIF1). Additionally, the presence of methylated PCR products was associated with absence of protein expression for the three genes and statistically significant for RASSF1A and WIF1. Interestingly, methylation of all the three genes was f

Materias

Biopsies

BRCAX

Hereditary breast cancer

Promoter hypermethylation

Protein expression

Tumor suppressor gene

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