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Structural studies of RFCCtf18 reveal a novel chromatin recruitment role for Dcc1

机译:RFCC的结构研究tf18揭示了Dcc1的新型染色质募集作用

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摘要

Replication factor C complexes load and unload processivity clamps from DNA and are involved in multiple DNA replication and repair pathways. The RFCC tf18 variant complex is required for activation of the intra‐S‐phase checkpoint at stalled replication forks and aids the establishment of sister chromatid cohesion. Unlike other RFC complexes, RFCC tf18 contains two non‐Rfc subunits, Dcc1 and Ctf8. Here, we present the crystal structure of the Dcc1‐Ctf8 heterodimer bound to the C‐terminus of Ctf18. We find that the C‐terminus of Dcc1 contains three‐winged helix domains, which bind to both ssDNA and dsDNA. We further show that these domains are required for full recruitment of the complex to chromatin, and correct activation of the replication checkpoint. These findings provide the first structural data on a eukaryotic seven‐subunit clamp loader and define a new biochemical activity for Dcc1.
机译:复制因子C复合物可从DNA加载和卸载合成钳位,并涉及多个DNA复制和修复途径。 RFC C tf18 变体复合体是激活停滞的复制叉处的S相检查点的必要条件,它有助于建立姐妹染色单体的内聚力。与其他RFC复合体不同,RFC C tf18 包含两个非Rfc子单元Dcc1和Ctf8。在这里,我们介绍了与Ctf18的C端结合的Dcc1-Ctf8异二聚体的晶体结构。我们发现,Dcc1的C末端包含三翼螺旋结构域,该结构域同时与ssDNA和dsDNA结合。我们进一步表明,这些结构域是将复合物完全募集到染色质以及正确激活复制检查点所必需的。这些发现为真核七亚基钳式装载机提供了第一批结构数据,并为Dcc1定义了新的生化活性。

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