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在单个着丝粒上对相互依赖且具有层级结构的动粒组装进行直接观察。

Direct observation of interdependent and hierarchical kinetochore assembly on individual centromeres.

作者信息

Hu Changkun, Popchock Andrew R, Latino Angelica Andrade, Asbury Charles L, Biggins Sue

机构信息

Basic Sciences Division, Howard Hughes Medical Institute, Fred Hutchinson Cancer Center, Seattle, WA, 98109 USA.

Department of Neurobiology and Biophysics, University of Washington, Seattle, WA, 98195 USA.

出版信息

bioRxiv. 2025 Jun 26:2025.06.25.661565. doi: 10.1101/2025.06.25.661565.

Abstract

Kinetochores are megadalton protein machines that harness microtubules to segregate chromosomes during cell division. The kinetochores must assemble after DNA replication during every cell cycle onto specialized regions of chromosomes called centromeres, but the order and regulation of their assembly remains unclear due to the complexity of kinetochore composition and the difficulty resolving individual kinetochores . Here, by adapting a prior single-molecule method for monitoring kinetochore assembly in budding yeast lysates, we identify a sequential order of assembly and uncover previously unknown interdependencies between subcomplexes. We show that inner kinetochore assembly depends partly on outer kinetochore components, and that outer kinetochore branches do not assemble independently of one another. Notably, Mif2 assembly is a rate-limiting step that can be accelerated by binding to the Mtw1 subcomplex, thereby promoting rapid assembly of many inner and outer kinetochore components. The importance of controlling kinetochore assembly kinetics is supported by a Mif2 mutant lacking both autoinhibition and Mtw1 subcomplex binding activity, which leads to defective kinetochore-microtubule attachments when the centromeric histone variant Cse4 is overexpressed. Altogether, our work provides a direct view of kinetochore assembly and reveals highly interdependent regulatory events that control its order and timing.

摘要

动粒是兆道尔顿级别的蛋白质机器,在细胞分裂过程中利用微管来分离染色体。在每个细胞周期的DNA复制后,动粒必须组装到染色体的特化区域——着丝粒上,但由于动粒组成的复杂性以及解析单个动粒的困难,其组装的顺序和调控仍不清楚。在这里,通过采用一种先前用于监测芽殖酵母裂解物中动粒组装的单分子方法,我们确定了组装的顺序,并揭示了亚复合物之间以前未知的相互依赖性。我们表明,内动粒的组装部分依赖于外动粒成分,并且外动粒分支并非彼此独立组装。值得注意的是,Mif2的组装是一个限速步骤,它可以通过与Mtw1亚复合物结合而加速,从而促进许多内、外动粒成分的快速组装。一个缺乏自抑制和Mtw1亚复合物结合活性的Mif2突变体支持了控制动粒组装动力学的重要性,当着丝粒组蛋白变体Cse4过表达时,该突变体会导致动粒 - 微管附着缺陷。总之,我们的工作提供了动粒组装的直接视图,并揭示了控制其顺序和时间的高度相互依赖的调控事件。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/75d4/12262613/ba5e94a85612/nihpp-2025.06.25.661565v1-f0002.jpg

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