Journal article
Analysis of RAD51C germline mutations in high-risk breast and ovarian cancer families and ovarian cancer patients
ER Thompson, SE Boyle, J Johnson, GL Ryland, S Sawyer, DYH Choong, undefined kConFab, G Chenevix-Trench, AH Trainer, GJ Lindeman, G Mitchell, PA James, IG Campbell
Human Mutation | WILEY-BLACKWELL | Published : 2012
DOI: 10.1002/humu.21625
Abstract
There is strong evidence that overtly inactivating mutations in RAD51C predispose to hereditary breast and ovarian cancer but the prevalence of such mutations, and whether they are associated with a particular clinical phenotype, remains unclear. Resolving these questions has important implications for the implementation of RAD51C into routine clinical genetic testing. Consequently, we have performed a large RAD51C mutation screen of hereditary breast and ovarian cancer families, and the first study of unselected patients diagnosed with ovarian cancer. Our data confirm a consistent but low frequency (2/335 families) of inactivating RAD51C mutations among families with a history of both breas..
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Awarded by National Breast Cancer Foundation
Awarded by Cancer Australia
Funding Acknowledgements
Contract grant sponsors: NHMRC; National Breast Cancer Foundation and Cancer Australia (#628333); Queensland Cancer Fund; The Cancer Councils of New South Wales, Victoria, Tasmania, and South Australia; The Cancer Foundation of Western Australia; Victorian Government via Victorian Cancer Agency; Cancer Australia and the National Breast Cancer Foundation (ID 628610).