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Ncd尾部与微管原纤维之间相互作用的结构分析。

A structural analysis of the interaction between ncd tail and tubulin protofilaments.

作者信息

Wendt Thomas, Karabay Arzu, Krebs Angelika, Gross Heinz, Walker Richard, Hoenger Andreas

机构信息

European Molecular Biology Laboratory, Meyerhofstrasse 1, 69117 Heidelberg, Germany.

出版信息

J Mol Biol. 2003 Oct 24;333(3):541-52. doi: 10.1016/j.jmb.2003.08.051.

Abstract

ncd is a minus-end directed, kinesin-like motor, which binds to microtubules with its motor domain and its cargo domain as well. Typical of retrograde motors, the motor domain of ncd locates to the C-terminal end of the polypeptide chain, and hence, the cargo domain constitutes the N-terminal region. To date, several studies have investigated the interaction properties of the motor domain with microtubules, but very few structural data are available about the tail itself or its interaction with microtubules as cargo. Here, we applied cryo-electron microscopy and helical 3D image reconstruction to 15 protofilament microtubules decorated with an ncd tail fragment (N-terminal residues 83-187, named NT6). In our study, the ncd tail shows a behaviour resembling filamentous MAPs such as tau protein, exhibiting a highly flexible structure with no large globular domains. NT6 binds to four different sites on the outer side of microtubules within the proximity of the kinesin motor-binding site. Two of these sites locate within the groove between two neighbouring protofilaments, and appear as strong binding sites, while the other two sites, located at the outer rim, appear to play a secondary role. In addition, the ncd tail fragment induces the formation of large protofilament sheets, suggesting a tail-induced modification of lateral protofilament contacts.

摘要

Ncd是一种向负端移动的、类似驱动蛋白的马达蛋白,它通过其马达结构域及其货物结构域与微管结合。与逆行马达蛋白一样,Ncd的马达结构域位于多肽链的C末端,因此,货物结构域构成N末端区域。迄今为止,已有多项研究探讨了马达结构域与微管的相互作用特性,但关于尾部本身或其作为货物与微管相互作用的结构数据却非常少。在这里,我们将冷冻电子显微镜和螺旋三维图像重建技术应用于由Ncd尾部片段(N末端残基83 - 187,命名为NT6)修饰的15根原纤维微管。在我们的研究中,Ncd尾部表现出类似于丝状微管相关蛋白(如tau蛋白)的行为,呈现出高度灵活的结构,没有大的球状结构域。NT6在驱动蛋白马达结合位点附近与微管外侧的四个不同位点结合。其中两个位点位于相邻两根原纤维之间的凹槽内,似乎是强结合位点,而另外两个位于外缘的位点似乎起次要作用。此外,Ncd尾部片段诱导形成大的原纤维片层,表明尾部诱导了原纤维侧向接触的改变。

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