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两步机制使中心体处微管组织中心功能失活。

A two-step mechanism for the inactivation of microtubule organizing center function at the centrosome.

机构信息

Department of Biology, Stanford University, Stanford, United States.

出版信息

Elife. 2019 Jun 27;8:e47867. doi: 10.7554/eLife.47867.

Abstract

The centrosome acts as a microtubule organizing center (MTOC), orchestrating microtubules into the mitotic spindle through its pericentriolar material (PCM). This activity is biphasic, cycling through assembly and disassembly during the cell cycle. Although hyperactive centrosomal MTOC activity is a hallmark of some cancers, little is known about how the centrosome is inactivated as an MTOC. Analysis of endogenous PCM proteins in revealed that the PCM is composed of partially overlapping territories organized into an inner and outer sphere that are removed from the centrosome at different rates and using different behaviors. We found that phosphatases oppose the addition of PCM by mitotic kinases, ultimately catalyzing the dissolution of inner sphere PCM proteins at the end of mitosis. The nature of the PCM appears to change such that the remaining aging PCM outer sphere is mechanically ruptured by cortical pulling forces, ultimately inactivating MTOC function at the centrosome.

摘要

中心体作为微管组织中心(MTOC),通过其中心粒周围物质(PCM)将微管组织成有丝分裂纺锤体。这种活性是双相的,在细胞周期中通过组装和拆卸循环进行。尽管过度活跃的中心体 MTOC 活性是一些癌症的标志,但对于中心体如何作为 MTOC 失活知之甚少。对 中内源性 PCM 蛋白的分析表明,PCM 由部分重叠的区域组成,分为内球和外球,它们以不同的速度和不同的行为从中心体上移除。我们发现,磷酸酶通过有丝分裂激酶来对抗 PCM 的添加,最终在有丝分裂末期催化内球 PCM 蛋白的溶解。PCM 的性质似乎发生了变化,使得剩余的老化 PCM 外球被皮质拉力机械性地破裂,最终使中心体的 MTOC 功能失活。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fa20/6684319/cf4163b98efd/elife-47867-fig1.jpg

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