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首页> 外文期刊>Molecular and Cellular Biology >Human RECQ1 and RECQ4 Helicases Play Distinct Roles in DNA Replication Initiation
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Human RECQ1 and RECQ4 Helicases Play Distinct Roles in DNA Replication Initiation

机译:人RECQ1和RECQ4解旋酶在DNA复制起始中起着不同的作用

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摘要

Cellular and biochemical studies support a role for all five human RecQ helicases in DNA replication; however, their specific functions during this process are unclear. Here we investigate the in vivo association of the five human RecQ helicases with three well-characterized human replication origins. We show that only RECQ1 (also called RECQL or RECQL1) and RECQ4 (also called RECQL4) associate with replication origins in a cell cycle-regulated fashion in unperturbed cells. RECQ4 is recruited to origins at late G1, after ORC and MCM complex assembly, while RECQ1 and additional RECQ4 are loaded at origins at the onset of S phase, when licensed origins begin firing. Both proteins are lost from origins after DNA replication initiation, indicating either disassembly or tracking with the newly formed replisome. Nascent-origin DNA synthesis and the frequency of origin firing are reduced after RECQ1 depletion and, to a greater extent, after RECQ4 depletion. Depletion of RECQ1, though not that of RECQ4, also suppresses replication fork rates in otherwise unperturbed cells. These results indicate that RECQ1 and RECQ4 are integral components of the human replication complex and play distinct roles in DNA replication initiation and replication fork progression in vivo.
机译:细胞和生化研究支持所有五种人类RecQ解旋酶在DNA复制中的作用。但是,在此过程中其具体功能尚不清楚。在这里,我们研究了五个人类RecQ解旋酶与三个特征明确的人类复制起点的体内关联。我们显示,只有RECQ1(也称为RECQL或RECQL1)和RECQ4(也称为RECQL4)在不受干扰的细胞中以细胞周期调控的方式与复制起点相关联。在ORC和MCM复合体组装后,RECQ4被招募到G 1 晚期的起源,而RECQ1和其他RECQ4在获得许可的起源开始发射时在S阶段开始时被加载。 DNA复制开始后,两种蛋白质都从起源中丢失,这表明它们已被重组或被新形成的复制体追踪。在RECQ1耗尽后,以及在更大程度上,在RECQ4耗尽后,新生鼻DNA的合成和原发频率降低。 RECQ1的耗尽(尽管不是RECQ4的耗尽)也抑制了原本不会受到干扰的单元中的复制派生速率。这些结果表明,RECQ1和RECQ4是人类复制复合物的组成部分,并且在DNA复制起始和体内复制叉进展中起着不同的作用。

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