Research Papers:
CHL1 hypermethylation as a potential biomarker of poor prognosis in breast cancer
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Abstract
Esperanza Martín-Sánchez1, Saioa Mendaza1, Ane Ulazia-Garmendia1, Iñaki Monreal-Santesteban1, Idoia Blanco-Luquin2, Alicia Córdoba3, Francisco Vicente-García4, Noemí Pérez-Janices1, David Escors2, Diego Megías5, Paula López-Serra6, Manel Esteller6,7,8, José Juan Illarramendi9, David Guerrero-Setas1,3
1Cancer Epigenetics Group, Navarrabiomed. Departmento de Salud-UPNA. IdiSNA, Pamplona, Spain
2Immunomodulation Group, Navarrabiomed. Departmento de Salud-UPNA. IdiSNA, Pamplona, Spain
3Department of Pathology, Complejo Hospitalario de Navarra, Servicio Navarro de Salud-Osasunbidea, Pamplona, Spain
4Department of Surgery, Complejo Hospitalario de Navarra, Servicio Navarro de Salud-Osasunbidea, Pamplona, Spain
5Confocal Microscopy Unit, Spanish National Cancer Research Centre, Madrid, Spain
6Cancer Epigenetics Group, Cancer Epigenetics and Biology Program, Bellvitge Biomedical Research Institute - IDIBELL, Barcelona, Spain
7Department of Physiological Sciences II, School of Medicine, University of Barcelona, Barcelona, Spain
8Institució Catalana de Recerca i Estudis Avançats (ICREA), Barcelona, Spain
9Department of Oncology, Complejo Hospitalario de Navarra, Servicio Navarro de Salud-Osasunbidea, Pamplona, Spain
Correspondence to:
Esperanza Martín-Sánchez, email: [email protected]
David Guerrero-Setas, email: [email protected]
Keywords: CHL1, DNA methylation, breast cancer, prognostic biomarker
Received: July 04, 2016 Accepted: January 03, 2017 Published: February 02, 2017
ABSTRACT
The CHL1 gene encodes a cell-adhesion molecule proposed as being a putative tumour-suppressor gene in breast cancer (BC). However, neither the underlying molecular mechanisms nor the clinical value of CHL1 downregulation in BC has been explored. The methylation status of three CpG sites in the CHL1 promoter was analysed by pyrosequencing in neoplastic biopsies from 142 patients with invasive BC and compared with that of non-neoplastic tissues. We found higher CHL1 methylation levels in breast tumours than in non-neoplastic tissues, either from mammoplasties or adjacent-to-tumour, which correlated with lower levels of protein expression in tumours measured by immunohistochemistry. A panel of five BC cell lines was treated with two epigenetic drugs, and restoration of CHL1 expression was observed, indicating in vitro dynamic epigenetic regulation. CHL1 was silenced by shRNA in immortalized but non-neoplastic mammary cells, and enhanced cell proliferation and migration, but not invasion, were found by real-time cell analysis. The prognostic value of CHL1 hypermethylation was assessed by the log-rank test and fitted in a Cox regression model. Importantly, CHL1 hypermethylation was very significantly associated with shorter progression-free survival in our BC patient series, independent of age and stage (p = 0.001). In conclusion, our results indicate that CHL1 is downregulated by hypermethylation and that this epigenetic alteration is an independent prognostic factor in BC.
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PII: 15004