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A mechanism of coupling RCC1 mobility to RanGTP production on the chromatin in vivo

机译:RCC1迁移率与体内染色质上RanGTP产生的耦合机制

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摘要

The RanGTP gradient across the interphase nuclear envelope and on the condensed mitotic chromosomes is essential for many cellular processes, including nucleocytoplasmic transport and spindle assembly. Although the chromosome-associated enzyme RCC1 is responsible for RanGTP production, the mechanism of generating and maintaining the RanGTP gradient in vivo remains unknown. Here, we report that regulator of chromosome condensation (RCC1) rapidly associates and dissociates with both interphase and mitotic chromosomes in living cells, and that this mobility is regulated during the cell cycle. Our kinetic modeling suggests that RCC1 couples its catalytic activity to chromosome binding to generate a RanGTP gradient. Indeed, we have demonstrated experimentally that the interaction of RCC1 with the chromatin is coupled to the nucleotide exchange on Ran in vivo. The coupling is due to the stable binding of the binary complex of RCC1–Ran to chromatin. Successful nucleotide exchange dissociates the binary complex, permitting the release of RCC1 and RanGTP from the chromatin and the production of RanGTP on the chromatin surface.
机译:RanGTP跨相间核包膜和浓缩的有丝分裂染色体上的梯度对于许多细胞过程(包括核质运输和纺锤体组装)至关重要。尽管染色体相关的酶RCC1负责RanGTP的产生,但在体内产生和维持RanGTP梯度的机制仍然未知。在这里,我们报告染色体浓缩调节剂(RCC1)与活细胞中的相间和有丝分裂染色体迅速关联和解离,并且这种迁移率在细胞周期中受到调节。我们的动力学模型表明,RCC1将其催化活性与染色体结合耦合以生成RanGTP梯度。实际上,我们已经通过实验证明了RCC1与染色质的相互作用与体内Ran上的核苷酸交换偶联。偶联是由于RCC1-Ran的二元复合物与染色质的稳定结合。成功的核苷酸交换可解离二元复合物,从而使RCC1和RanGTP从染色质释放,并在染色质表面上产生RanGTP。

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