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Coordinated protein and DNA remodeling by human HLTF on stalled replication fork

机译:人类HLTF在停滞的复制叉上协调的蛋白质和DNA重塑

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摘要

Human helicase-like transcription factor (HLTF) exhibits ubiquitin ligase activity for proliferating cell nuclear antigen (PCNA) polyu-biquityfation as well as double-stranded DNA translocase activity for remodeling stalled replication fork by fork reversal, which can support damage bypass by template switching. However, a stalled replication fork is surrounded by various DNA-binding proteins which can inhibit the access of damage bypass players, and it is unknown how these proteins become displaced. Here we reveal that HLTF has an ATP hydrolysis-dependent protein remodeling activity, by which it can remove proteins bound to the replication fork. Moreover, we demonstrate that HLTF can displace a broad spectrum of proteins such as replication protein A (RPA), PCNA, and replication factor C (RFC), thereby providing the first example for a protein clearing activity at the stalled replication fork. Our findings clarify how remodeling of a stalled replication fork can occur if it is engaged in interactions with masses of proteins.
机译:人类解旋酶样转录因子(HLTF)表现出泛素连接酶活性,用于增殖细胞核抗原(PCNA)多聚泛素化,以及双链DNA转移酶活性,用于通过叉子逆转来重构停滞的复制叉子,这可以通过模板切换来支持损伤旁路。但是,停滞的复制叉被各种DNA结合蛋白所包围,这些蛋白可以抑制损伤旁路分子的进入,并且未知这些蛋白如何被置换。在这里,我们揭示了HLTF具有ATP水解依赖的蛋白质重塑活性,通过它可以去除与复制叉结合的蛋白质。此外,我们证明了HLTF可以取代广谱的蛋白质,例如复制蛋白A(RPA),PCNA和复制因子C(RFC),从而为停滞的复制叉中的蛋白质清除活性提供了第一个例子。我们的发现阐明了停滞的复制叉如果与大量蛋白质相互作用,将如何发生重塑。

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    Institute of Genetics, Biological Research Center, Hungarian Academy of Sciences, Temesvari krt.62, H-6726, Szeged, Hungary;

    Institute of Genetics, Biological Research Center, Hungarian Academy of Sciences, Temesvari krt.62, H-6726, Szeged, Hungary;

    Institute of Genetics, Biological Research Center, Hungarian Academy of Sciences, Temesvari krt.62, H-6726, Szeged, Hungary;

  • 收录信息 美国《科学引文索引》(SCI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
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  • 正文语种 eng
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  • 入库时间 2022-08-18 00:40:53

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