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Data from Functionally Null RAD51D Missense Mutation Associates Strongly with Ovarian Carcinoma

Posted on 2023-03-31 - 00:46
Abstract

RAD51D is a key player in DNA repair by homologous recombination (HR), and RAD51D truncating variant carriers have an increased risk for ovarian cancer. However, the contribution of nontruncating RAD51D variants to cancer predisposition remains uncertain. Using deep sequencing and case–control genotyping studies, we show that in French Canadians, the missense RAD51D variant c.620C>T;p.S207L is highly prevalent and is associated with a significantly increased risk for ovarian high-grade serous carcinoma (HGSC; 3.8% cases vs. 0.2% controls). The frequency of the p.S207L variant did not significantly differ from that of controls in breast, endometrial, pancreas, or colorectal adenocarcinomas. Functionally, we show that this mutation impairs HR by disrupting the RAD51D–XRCC2 interaction and confers PARP inhibitor sensitivity. These results highlight the importance of a functional RAD51D–XRCC2 interaction to promote HR and prevent the development of HGSC. This study identifies c.620C>T;p.S207L as the first bona fide pathogenic RAD51D missense cancer susceptibility allele and supports the use of targeted PARP-inhibitor therapies in ovarian cancer patients carrying deleterious missense RAD51D variants. Cancer Res; 77(16); 4517–29. ©2017 AACR.

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FUNDING

Quebec Breast Cancer Foundation

Susan G. Komen

Canadian Institutes of Health Research

CIHR

Cancer Research Society of Canada

Canadian Cancer Society Research Institute

Cancer Research UK

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AUTHORS (32)

  • Barbara Rivera
    Massimo Di Iorio
    Jessica Frankum
    Javad Nadaf
    Somayyeh Fahiminiya
    Suzanna L. Arcand
    David L. Burk
    Damien Grapton
    Eva Tomiak
    Valerie Hastings
    Nancy Hamel
    Rabea Wagener
    Olga Aleynikova
    Sylvie Giroux
    Fadi F. Hamdan
    Alexandre Dionne-Laporte
    George Zogopoulos
    Francois Rousseau
    Albert M. Berghuis
    Diane Provencher
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