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HA95 and LAP2β mediate a novel chromatin–nuclear envelope interaction implicated in initiation of DNA replication

机译:HA95和LAP2β介导新的染色质-核包膜相互作用与DNA复制的启动有关

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摘要

HA95 is a chromatin-associated protein that interfaces the nuclear envelope (NE) and chromatin. We report an interaction between HA95 and the inner nuclear membrane protein lamina-associated polypeptide (LAP) 2β, and a role of this association in initiation of DNA replication. Precipitation of GST–LAP2β fusion proteins and overlays of immobilized HA95 indicate that a first HA95-binding region lies within amino acids 137–242 of LAP2β. A second domain sufficient to bind HA95 colocalizes with the lamin B–binding domain of LAP2β at residues 299–373. HA95–LAP2β interaction is not required for NE formation. However, disruption of the association of HA95 with the NH2-terminal HA95-binding domain of LAP2β abolishes the initiation, but not elongation, of DNA replication in purified G1 phase nuclei incubated in S-phase extract. Inhibition of replication initiation correlates with proteasome-mediated proteolysis of Cdc6, a component of the prereplication complex. Rescue of Cdc6 degradation with proteasome inhibitors restores replication. We propose that an interaction of LAP2β, or LAP2 proteins, with HA95 is involved in the control of initiation of DNA replication.
机译:HA95是与染色质相关的蛋白,可与核膜(NE)和染色质连接。我们报告了HA95和内核膜蛋白层状相关多肽(LAP)2β之间的相互作用,以及这种联系在DNA复制起始中的作用。 GST-LAP2β融合蛋白的沉淀和固定的HA95的覆盖物表明,第一个HA95结合区位于LAP2β的137-242位氨基酸内。足以结合HA95的第二个结构域与LAP2β的lamin B结合结构域在299-373位残基共定位。 NE形成不需要HA95–LAP2β相互作用。但是,HA95与LAP2β的NH2末端HA95结合域的结合的破坏消除了在S期提取物中培养的纯化G1期核中DNA复制的起始,但没有延长。复制起始的抑制与蛋白酶体介导的Cdc6的蛋白水解有关,Cdc6是复制前复合物的组成部分。用蛋白酶体抑制剂拯救Cdc6降解可恢复复制。我们建议与HA95的LAP2β或LAP2蛋白质的相互作用涉及DNA复制起始的控制。

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