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首页> 外文期刊>Cell cycle >New advances in the DNA damage response network of Fanconi anemia and BRCA proteins. FAAP95 replaces BRCA2 as the true FANCB protein.
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New advances in the DNA damage response network of Fanconi anemia and BRCA proteins. FAAP95 replaces BRCA2 as the true FANCB protein.

机译:Fanconi贫血和BRCA蛋白的DNA损伤反应网络的新进展。 FAAP95取代BRCA2作为真正的FANCB蛋白。

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摘要

Fanconi anemia (FA) proteins function in a DNA damage response pathway that appears to be part of the network including breast cancer susceptibility gene products, BRCA1 and BRCA2. In response to DNA damage or replication signals, a nuclear FA core complex of at least 6 FA proteins (FANCA, FANCC, FANCE, FANCF, FANCG and FANCL) is activated and leads to monoubiquitination of the downstream FA protein, FANCD2. One puzzling question for this pathway is the role of BRCA2. A previous study has proposed that BRCA2 could be identical to two FA proteins: FANCD1, which functions either downstream or in a parallel pathway; and FANCB, which functions upstream of the FANCD2 monoubiquitination. Now, a new study shows that the real FANCB protein is not BRCA2, but a previously uncharacterized component of the FA core complex, FAAP95, suggesting that BRCA2 does not act upstream of the FA pathway. Interestingly, the newly discovered FANCB gene is X-linked and subject to X-inactivation. The presence of a single active copy of FANCB and its essentiality for a functional FA-BRCA pathway make it a potentially vulnerable component of the cellular machinery that maintains genomic integrity.
机译:范可尼贫血(FA)蛋白在DNA损伤反应途径中起作用,该途径似乎是该网络的一部分,包括乳腺癌易感性基因产物BRCA1和BRCA2。响应DNA损伤或复制信号,至少6种FA蛋白(FANCA,FANCC,FANCE,FANCF,FANCG和FANCL)的核FA核心复合物被激活,并导致下游FA蛋白FANCD2单泛素化。此途径的一个令人困惑的问题是BRCA2的作用。先前的研究提出BRCA2可能与两种FA蛋白相同:FANCD1,其在下游或平行途径中起作用;和FANCB,其在FANCD2单泛素化上游起作用。现在,一项新的研究表明,真正的FANCB蛋白不是BRCA2,而是FA核心复合体FAAP95以前未知的成分,这表明BRCA2并不在FA途径的上游起作用。有趣的是,新发现的FANCB基因是X连锁的,并且会X灭活。 FANCB的单个有效拷贝的存在及其对功能性FA-BRCA途径的必要性使其成为维持基因组完整性的细胞机械的潜在脆弱组分。

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