Mutation screening of RAD51C in high-risk breast and ovarian cancer families

被引:0
|
作者
Wenping Lu
Xianshu Wang
Hongsheng Lin
Noralane M. Lindor
Fergus J. Couch
机构
[1] China Academy of Chinese Medical Sciences,Oncology Department of Guang’anmen Hospital
[2] Mayo Clinic College of Medicine,Department of Laboratory Medicine and Pathology
[3] Mayo Clinic College of Medicine,Department of Medical Genetics
来源
Familial Cancer | 2012年 / 11卷
关键词
Mutation screening; Familial breast and ovarian cancer; Breast cancer predisposition;
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学科分类号
摘要
Deleterious mutations in the RAD51C gene, which encodes a DNA double-strand break repair protein, have been reported to confer high-penetrance susceptibility to both breast and ovarian cancer. To confirm this we conducted a mutation screen of the RAD51C gene in 192 probands from high-risk breast and/or ovarian cancer families that do not carry BRCA1 or BRCA2 mutations. The nine exons of the RAD51C gene containing protein coding sequence were screened for mutations in genomic DNA from family probands by high-resolution melting analysis and direct DNA sequencing. Four missense variants, p.Ser364Gly, p.Ala126Thr, p.Val169Ala, and p.Thr287Ala were detected in six patients. The p.Ser364Gly variant is a novel variant predicted to have little influence on RAD51C activity. The p.Ala126Thr and p.Val169Ala variants have been reported to have no association with risk of breast cancer in a case–control study. However, p.Thr287Ala disrupts the DNA repair activity of RAD51C, suggesting some influence on risk. Consistent with published results from similar follow-up studies, we suggest that RAD51C mutations are rare events among high-risk breast cancer and breast/ovarian cancer families. Large population-based studies will be needed to reliably assess the prevalence and penetrance of inactivating mutations in the RAD51C susceptibility gene.
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页码:381 / 385
页数:4
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