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动力蛋白 KIF5B 和 KIF13B 的协同作用促进了高效的分泌囊泡向微管正极的运输。

Concerted action of kinesins KIF5B and KIF13B promotes efficient secretory vesicle transport to microtubule plus ends.

机构信息

Cell Biology, Neurobiology and Biophysics, Department of Biology, Faculty of Science, Utrecht University, Utrecht, Netherlands.

Departments of Medical Informatics and Radiology, Biomedical Imaging Group Rotterdam, Erasmus University Medical Center, Rotterdam, Netherlands.

出版信息

Elife. 2020 Nov 11;9:e61302. doi: 10.7554/eLife.61302.

Abstract

Intracellular transport relies on multiple kinesins, but it is poorly understood which kinesins are present on particular cargos, what their contributions are and whether they act simultaneously on the same cargo. Here, we show that Rab6-positive secretory vesicles are transported from the Golgi apparatus to the cell periphery by kinesin-1 KIF5B and kinesin-3 KIF13B, which determine the location of secretion events. KIF5B plays a dominant role, whereas KIF13B helps Rab6 vesicles to reach freshly polymerized microtubule ends, to which KIF5B binds poorly, likely because its cofactors, MAP7-family proteins, are slow in populating these ends. Sub-pixel localization demonstrated that during microtubule plus-end directed transport, both kinesins localize to the vesicle front and can be engaged on the same vesicle. When vesicles reverse direction, KIF13B relocates to the middle of the vesicle, while KIF5B shifts to the back, suggesting that KIF5B but not KIF13B undergoes a tug-of-war with a minus-end directed motor.

摘要

细胞内运输依赖于多种驱动蛋白,但对于特定货物上存在哪些驱动蛋白、它们的贡献是什么以及它们是否同时作用于同一货物,人们知之甚少。在这里,我们表明 Rab6 阳性分泌囊泡由驱动蛋白-1 KIF5B 和驱动蛋白-3 KIF13B 从高尔基体运输到细胞边缘,这决定了分泌事件的位置。KIF5B 起主导作用,而 KIF13B 帮助 Rab6 囊泡到达新聚合的微管末端,KIF5B 与这些末端结合不良,可能是因为其辅助因子 MAP7 家族蛋白在这些末端的募集速度较慢。亚像素定位表明,在微管正极导向运输过程中,两种驱动蛋白都定位于囊泡前端,并且可以在同一个囊泡上结合。当囊泡反转方向时,KIF13B 重新定位到囊泡的中间,而 KIF5B 转移到后端,这表明 KIF5B 而不是 KIF13B 与向负极定向的马达发生拔河。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d4d3/7710357/d9b414afa7b1/elife-61302-fig1.jpg

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