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Genetic instability in the RAD51 and BRCA1 regions in breast cancer

机译:乳腺癌RAD51和BRCA1区的遗传不稳定性

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摘要

Breast cancer is the most prevalent cancer type in women. Accumulating evidence indicates that the fidelity of double-strand break repair in response to DNA damage is an important step in mammary neoplasias. The RAD51 and BRCA1 proteins are involved in the repair of double-strand DNA breaks by homologous recombination. In this study, we evaluated loss of heterozygosity (LOH) in the RAD51 and BRCA1 regions, and their association with breast cancer. The polymorphic markers D15S118, D15S214 and D15S1006 were the focus for RAD51, and D17S855 and D17S1323 for BRCA1. Genomic deletion detected by allelic loss varied according to the regions tested, and ranged from 29 to 46% of informative cases for the RAD51 region and from 38 to 42% of informative cases for the BRCA1 region. 25% of breast cancer cases displayed LOH for at least one studied marker in the RAD51 region exclusively. On the other hand, 31% of breast cancer cases manifested LOH for at least one microsatellite marker concomitantly in the RAD51 and BRCA1 regions. LOH in the RAD51 region, similarly as in the BRCA1 region, appeared to correlate with steroid receptor status. The obtained results indicate that alteration in the RAD51 region may contribute to the disturbances of DNA repair involving RAD51 and BRCA1 and thus enhance the risk of breast cancer development.
机译:乳腺癌是女性中最普遍的癌症类型。越来越多的证据表明,对DNA损伤作出反应的双链断裂修复的保真度是乳腺肿瘤的重要一步。 RAD51和BRCA1蛋白通过同源重组参与双链DNA断裂的修复。在这项研究中,我们评估了RAD51和BRCA1区杂合性(LOH)的丧失,以及它们与乳腺癌的关系。多态性标记D15S118,D15S214和D15S1006是RAD51的焦点,而D17S855和D17S1323是BRCA1的焦点。通过等位基因缺失检测到的基因组缺失根据所测试的区域而异,对于RAD51区而言,占情报病例的29%至46%,对于BRCA1区而言,占情报病例的38%至42%。 25%的乳腺癌病例仅在RAD51区域中至少显示一种研究标记的LOH。另一方面,31%的乳腺癌病例在RAD51和BRCA1区同时伴有至少一个微卫星标志物的LOH。与BRCA1区类似,RAD51区的LOH似乎与类固醇受体状态相关。获得的结果表明,RAD51区的改变可能会导致涉及RAD51和BRCA1的DNA修复紊乱,从而增加患乳腺癌的风险。

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