BRCA2 Carriers with Male Breast Cancer Show Elevated Tumour Methylation

Overview

Journal BMC Cancer

Publisher Biomed Central

Specialty Oncology

Date 2017 Sep 13

PMID 28893223

Citations 8

Authors

Siddhartha Deb

Kylie L Gorringe

Jia-Min B Pang

David J Byrne

Elena A Takano

Alexander Dobrovic

Stephen B Fox

Affiliations

Soon will be listed here.

Abstract

Background: Male breast cancer (MBC) represents a poorly characterised group of tumours, the management of which is largely based on practices established for female breast cancer. However, recent studies demonstrate biological and molecular differences likely to impact on tumour behaviour and therefore patient outcome. The aim of this study was to investigate methylation of a panel of commonly methylated breast cancer genes in familial MBCs.

Methods: 60 tumours from 3 BRCA1 and 25 BRCA2 male mutation carriers and 32 males from BRCAX families were assessed for promoter methylation by methylation-sensitive high resolution melting in a panel of 10 genes (RASSF1A, TWIST1, APC, WIF1, MAL, RARβ, CDH1, RUNX3, FOXC1 and GSTP1). An average methylation index (AMI) was calculated for each case comprising the average of the methylation of the 10 genes tested as an indicator of overall tumour promoter region methylation. Promoter hypermethylation and AMI were correlated with BRCA carrier mutation status and clinicopathological parameters including tumour stage, grade, histological subtype and disease specific survival.

Results: Tumours arising in BRCA2 mutation carriers showed significantly higher methylation of candidate genes, than those arising in non-BRCA2 familial MBCs (average AMI 23.6 vs 16.6, p = 0.01, 45% of genes hypermethylated vs 34%, p < 0.01). RARβ methylation and AMI-high status were significantly associated with tumour size (p = 0.01 and p = 0.02 respectively), RUNX3 methylation with invasive carcinoma of no special type (94% vs 69%, p = 0.046) and RASSF1A methylation with coexistence of high grade ductal carcinoma in situ (33% vs 6%, p = 0.02). Cluster analysis showed MBCs arising in BRCA2 mutation carriers were characterised by RASSF1A, WIF1, RARβ and GTSP1 methylation (p = 0.02) whereas methylation in BRCAX tumours showed no clear clustering to particular genes. TWIST1 methylation (p = 0.001) and AMI (p = 0.01) were prognostic for disease specific survival.

Conclusions: Increased methylation defines a subset of familial MBC and with AMI may be a useful prognostic marker. Methylation might be predictive of response to novel therapeutics that are currently under investigation in other cancer types.

Citing Articles

Male Breast Cancer: An Updated Review of Patient Characteristics, Genetics, and Outcome.

Khare V, Huda F, Misra S, Amulya K, Raj N, Karn S Int J Breast Cancer. 2024; 2024:9003572.

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() Gene Methylation in Human Breast Cancer: Critical Appraisal of a Long and Twisted Story.

Bucker L, Lehmann U Cancers (Basel). 2022; 14(18).

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Analysis of the Clinical Advancements for -Related Malignancies Highlights the Lack of Treatment Evidence for -Positive Male Breast Cancer.

McClurg D, Urquhart G, McGoldrick T, Chatterji S, Miedzybrodzka Z, Speirs V Cancers (Basel). 2022; 14(13).

PMID: 35804947 PMC: 9264767. DOI: 10.3390/cancers14133175.

Male Breast Cancer: From Molecular Genetics to Clinical Management.

Pensabene M, von Arx C, De Laurentiis M Cancers (Basel). 2022; 14(8).

PMID: 35454911 PMC: 9030724. DOI: 10.3390/cancers14082006.

DNA methylation variations in familial female and male breast cancer.

Abeni E, Grossi I, Marchina E, Coniglio A, Incardona P, Cavalli P Oncol Lett. 2021; 21(6):468.

PMID: 33907578 PMC: 8063268. DOI: 10.3892/ol.2021.12729.

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