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Replication protein A phosphorylation and the cellular response to DNA damage.

机译:复制蛋白A磷酸化和细胞对DNA损伤的反应。

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摘要

Defects in cellular DNA metabolism have a direct role in many human disease processes. Impaired responses to DNA damage and basal DNA repair have been implicated as causal factors in diseases with DNA instability like cancer, Fragile X and Huntington's. Replication protein A (RPA) is essential for multiple processes in DNA metabolism including DNA replication, recombination and DNA repair pathways (including nucleotide excision, base excision and double-strand break repair). RPA is a single-stranded DNA-binding protein composed of subunits of 70-, 32- and 14-kDa. RPA binds ssDNA with high affinity and interacts specifically with multiple proteins. Cellular DNA damage causes the N-terminus of the 32-kDa subunit of human RPA to become hyper-phosphorylated. Current data indicates that hyper-phosphorylation causes a change in RPA conformation that down-regulates activity in DNA replication but does not affect DNA repair processes. This suggests that the role of RPA phosphorylation in the cellular response to DNA damage is to help regulate DNA metabolism and promote DNA repair.
机译:细胞DNA代谢缺陷在许多人类疾病过程中具有直接作用。对DNA损伤和基础DNA修复的反应减弱已被认为是诸如癌症,易碎X和亨廷顿病等具有DNA不稳定性的疾病的病因。复制蛋白A(RPA)对于DNA代谢的多个过程至关重要,包括DNA复制,重组和DNA修复途径(包括核苷酸切除,碱基切除和双链断裂修复)。 RPA是由70-,32-和14-kDa的亚基组成的单链DNA结合蛋白。 RPA以高亲和力结合ssDNA,并与多种蛋白质特异性相互作用。细胞DNA的破坏会导致人RPA的32 kDa亚基的N端过度磷酸化。当前数据表明,过度磷酸化会引起RPA构象的改变,从而下调DNA复制中的活性,但不影响DNA修复过程。这表明RPA磷酸化在细胞对DNA损伤的反应中的作用是帮助调节DNA代谢并促进DNA修复。

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