A Genome-wide Association Study for Malignant Mesothelioma Risk

Overview

Journal Lung Cancer

Specialty Oncology

Date 2013 Jul 6

PMID 23827383

Citations 19

Authors

Gemma Cadby

Sutapa Mukherjee

A W Bill Musk

Alison Reid

Mike Garlepp

Ian Dick

Cleo Robinson

Jennie Hui

Giovanni Fiorito

Simonetta Guarrera

John Beilby

Phillip E Melton

Eric K Moses

Donatella Ugolini

Dario Mirabelli

Stefano Bonassi

Corrado Magnani

Irma Dianzani

Giuseppe Matullo

Bruce Robinson

Jenette Creaney

Lyle J Palmer

Affiliations

Soon will be listed here.

Abstract

Malignant mesothelioma (MM) is a uniformly fatal tumour of mesothelial cells. MM is caused by exposure to asbestos however most individuals with documented asbestos exposure do not develop MM. Although MM appears to aggregate within families, the genetics of MM susceptibility is a relatively unexplored area. The aim of the current study was to identify genetic factors that contribute to MM risk. A genome-wide association analysis of 2,508,203 single nucleotide polymorphisms (SNPs) from 428 MM cases and 1269 controls from Western Australia was performed. Additional genotyping was performed on a sample of 778 asbestos-exposed Western Australian controls. Replication of the most strongly associated SNPs was undertaken in an independent case-control study of 392 asbestos-exposed cases and 367 asbestos-exposed controls from Italy. No SNPs achieved formal genome-wide statistical significance in the Western Australian study. However, suggestive results for MM risk were identified in the SDK1, CRTAM and RASGRF2 genes, and in the 2p12 chromosomal region. These findings were not replicated in the Italian study, although there was some evidence of replication in the region of SDK1. These suggestive associations will be further investigated in sequencing and functional studies.

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