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动力蛋白-动力蛋白激活蛋白-NuMA复合物激活与调控的结构和功能见解

Structural and functional insights into activation and regulation of the dynein-dynactin-NuMA complex.

作者信息

Aslan Merve, d'Amico Ennio A, Cho Nathan H, Taheri Aryan, Zhao Yuanchang, Zhong Xinyue, Blaauw Madeline, Carter Andrew P, Dumont Sophie, Yildiz Ahmet

出版信息

bioRxiv. 2024 Dec 3:2024.11.26.625568. doi: 10.1101/2024.11.26.625568.

Abstract

During cell division, NuMA orchestrates the focusing of microtubule minus-ends in spindle poles and cortical force generation on astral microtubules by interacting with dynein motors, microtubules, and other cellular factors. Here we used in vitro reconstitution, cryo-electron microscopy, and live cell imaging to understand the mechanism and regulation of NuMA. We determined the structure of the processive dynein/dynactin/NuMA complex (DDN) and showed that the NuMA N-terminus drives dynein motility in vitro and facilitates dynein-mediated transport in live cells. The C-terminus of NuMA directly binds to and suppresses the dynamics of the microtubule minus-end. Full-length NuMA is autoinhibited, but mitotically phosphorylated NuMA activates dynein in vitro and interphase cells. Together with dynein, activated full-length NuMA focuses microtubule minus-ends into aster-like structures. The binding of the cortical protein LGN to the NuMA C-terminus results in preferential binding of NuMA to the microtubule plus-end. These results provide critical insights into the activation of NuMA and dynein for their functions in the spindle body and the cell cortex.

摘要

在细胞分裂过程中,核有丝分裂器蛋白(NuMA)通过与动力蛋白、微管及其他细胞因子相互作用,协调纺锤体极中微管负端的聚焦以及星状微管上皮质力的产生。在此,我们运用体外重建、冷冻电子显微镜及活细胞成像技术来了解NuMA的作用机制及调控方式。我们确定了前进动力蛋白/动力蛋白激活蛋白/NuMA复合物(DDN)的结构,并表明NuMA的N端在体外驱动动力蛋白运动,并促进活细胞中动力蛋白介导的运输。NuMA的C端直接结合并抑制微管负端的动态变化。全长NuMA处于自身抑制状态,但有丝分裂期磷酸化的NuMA在体外和间期细胞中激活动力蛋白。激活的全长NuMA与动力蛋白一起将微管负端聚焦成星状结构。皮质蛋白LGN与NuMA C端的结合导致NuMA优先结合到微管正端。这些结果为NuMA和动力蛋白在纺锤体和细胞皮质中的功能激活提供了关键见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/519f/11623564/7bf4a2725248/nihpp-2024.11.26.625568v2-f0008.jpg

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