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FAP206是一种用于纤毛辐条2和动力蛋白c的微管对接衔接蛋白。

FAP206 is a microtubule-docking adapter for ciliary radial spoke 2 and dynein c.

作者信息

Vasudevan Krishna Kumar, Song Kangkang, Alford Lea M, Sale Winfield S, Dymek Erin E, Smith Elizabeth F, Hennessey Todd, Joachimiak Ewa, Urbanska Paulina, Wloga Dorota, Dentler William, Nicastro Daniela, Gaertig Jacek

机构信息

Department of Cellular Biology, University of Georgia, Athens, GA 30602.

Department of Biology, Rosenstiel Center, Brandeis University, Waltham, MA 02454.

出版信息

Mol Biol Cell. 2015 Feb 15;26(4):696-710. doi: 10.1091/mbc.E14-11-1506. Epub 2014 Dec 24.

Abstract

Radial spokes are conserved macromolecular complexes that are essential for ciliary motility. A triplet of three radial spokes, RS1, RS2, and RS3, repeats every 96 nm along the doublet microtubules. Each spoke has a distinct base that docks to the doublet and is linked to different inner dynein arms. Little is known about the assembly and functions of individual radial spokes. A knockout of the conserved ciliary protein FAP206 in the ciliate Tetrahymena resulted in slow cell motility. Cryo-electron tomography showed that in the absence of FAP206, the 96-nm repeats lacked RS2 and dynein c. Occasionally, RS2 assembled but lacked both the front prong of its microtubule base and dynein c, whose tail is attached to the front prong. Overexpressed GFP-FAP206 decorated nonciliary microtubules in vivo. Thus FAP206 is likely part of the front prong and docks RS2 and dynein c to the microtubule.

摘要

径向辐条是保守的大分子复合物,对纤毛运动至关重要。由三条径向辐条RS1、RS2和RS3组成的三联体沿着双联微管每96纳米重复一次。每条辐条都有一个独特的基部,该基部与双联微管对接,并与不同的内动力蛋白臂相连。关于单个径向辐条的组装和功能知之甚少。在纤毛虫四膜虫中敲除保守的纤毛蛋白FAP206会导致细胞运动缓慢。冷冻电子断层扫描显示,在缺乏FAP206的情况下,96纳米的重复结构缺少RS2和动力蛋白c。偶尔,RS2会组装,但缺少其微管基部的前叉以及动力蛋白c,动力蛋白c的尾部附着在前叉上。体内过表达的GFP-FAP206修饰了非纤毛微管。因此,FAP206可能是前叉的一部分,并将RS2和动力蛋白c对接至微管。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d322/4325840/0de1696ae80f/696fig1.jpg

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