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首页> 外文期刊>The Veterinary Journal >Interactions between canine RAD51 and full length or truncated BRCA2 BRC repeats.
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Interactions between canine RAD51 and full length or truncated BRCA2 BRC repeats.

机译:犬RAD51与全长或截短的BRCA2 BRC重复序列之间的相互作用。

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摘要

In humans, mutations in the gene for the breast cancer susceptibility protein BRCA2 affect its interactions with the recombinase RAD51 and are associated with an increased risk of cancer. This interaction occurs through a series of eight BRC repeat sequences in BRCA2. A mammalian two-hybrid assay using individual BRC repeats demonstrated that BRC6 did not bind to RAD51, whereas there was strong (BRC1, 2 and 4), intermediate (BRC8), or weak (BRC3, 5 and 7) binding of other BRC repeats to RAD51. In serial deletion mutation experiments, binding strengths were increased when the C-terminal BRC repeat was removed from BRC1-8, BRC1-5 and BRC1-3. These results may provide an insight into the effects of missense or truncation mutations in BRCA2 in canine tumours.Digital Object Identifier http://dx.doi.org/10.1016/j.tvjl.2010.11.001
机译:在人类中,乳腺癌敏感性蛋白BRCA2的基因突变会影响其与重组酶RAD51的相互作用,并增加患癌的风险。这种相互作用是通过BRCA2中的一系列八个BRC重复序列发生的。使用单个BRC重复序列的哺乳动物双杂交试验表明,BRC6不与RAD51结合,而其他BRC重复序列的结合强度高(BRC1、2和4),中间(BRC8)或弱(BRC3、5和7)。到RAD51。在系列缺失突变实验中,当从BRC1-8,BRC1-5和BRC1-3中去除C端BRC重复序列时,结合强度会提高。这些结果可提供深入了解BRCA2的错义或截短突变对犬肿瘤的影响的信息。数字对象标识符http://dx.doi.org/10.1016/j.tvjl.2010.11.001

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