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驱动蛋白-4 KIF21B是一种强大的微管暂停因子。

Kinesin-4 KIF21B is a potent microtubule pausing factor.

作者信息

van Riel Wilhelmina E, Rai Ankit, Bianchi Sarah, Katrukha Eugene A, Liu Qingyang, Heck Albert Jr, Hoogenraad Casper C, Steinmetz Michel O, Kapitein Lukas C, Akhmanova Anna

机构信息

Cell Biology, Department of Biology, Faculty of Science, Utrecht University, Utrecht, Netherlands.

Laboratory of Biomolecular Research, Department of Biology and Chemistry, Paul Scherrer Institut, Villigen PSI, Switzerland.

出版信息

Elife. 2017 Mar 14;6:e24746. doi: 10.7554/eLife.24746.

Abstract

Microtubules are dynamic polymers that in cells can grow, shrink or pause, but the factors that promote pausing are poorly understood. Here, we show that the mammalian kinesin-4 KIF21B is a processive motor that can accumulate at microtubule plus ends and induce pausing. A few KIF21B molecules are sufficient to induce strong growth inhibition of a microtubule plus end in vitro. This property depends on non-motor microtubule-binding domains located in the stalk region and the C-terminal WD40 domain. The WD40-containing KIF21B tail displays preference for a GTP-type over a GDP-type microtubule lattice and contributes to the interaction of KIF21B with microtubule plus ends. KIF21B also contains a motor-inhibiting domain that does not fully block the interaction of the protein with microtubules, but rather enhances its pause-inducing activity by preventing KIF21B detachment from microtubule tips. Thus, KIF21B combines microtubule-binding and regulatory activities that together constitute an autonomous microtubule pausing factor.

摘要

微管是动态聚合物,在细胞中可生长、收缩或暂停,但促进暂停的因素却知之甚少。在此,我们表明哺乳动物驱动蛋白-4 KIF21B是一种持续运动蛋白,可在微管正端积累并诱导暂停。少数KIF21B分子足以在体外诱导微管正端强烈的生长抑制。这一特性取决于位于柄部区域和C端WD40结构域的非运动性微管结合结构域。含WD40的KIF21B尾部对GTP型微管晶格的偏好超过GDP型微管晶格,并有助于KIF21B与微管正端的相互作用。KIF21B还包含一个运动抑制结构域,该结构域不会完全阻断该蛋白与微管的相互作用,而是通过防止KIF21B从微管尖端脱离来增强其诱导暂停的活性。因此,KIF21B结合了微管结合和调节活性,共同构成一个自主的微管暂停因子。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5063/5383399/202b5899c7b0/elife-24746-fig1.jpg

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