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在来自布氏锥虫的一种高分子量微管相关蛋白中鉴定出的一种新型微管结合基序。

A novel microtubule-binding motif identified in a high molecular weight microtubule-associated protein from Trypanosoma brucei.

作者信息

Hemphill A, Affolter M, Seebeck T

机构信息

Institute for General Microbiology, University of Bern, Switzerland.

出版信息

J Cell Biol. 1992 Apr;117(1):95-103. doi: 10.1083/jcb.117.1.95.

Abstract

The major component of the cytoskeleton of the parasitic hemoflagellate Trypanosoma brucei is a membrane skeleton which consists of a single layer of tightly spaced microtubules. This array encloses the entire cell body, and it is apposed to, and connected with, the overlying cell membrane. The microtubules of this array contain numerous microtubule-associated proteins. Prominent among those is a family of high molecular weight, repetitive proteins which consist to a large extent of tandemly arranged 38-amino acid repeat units. The binding of one of these proteins, MARP-1, to microtubules has now been characterized in vitro and in vivo. MARP-1 binds to microtubules via tubulin domains other than the COOH-termini used by microtubule-associated proteins from mammalian brain, e.g., MAP2 or Tau. In vitro binding assays using recombinant protein, as well as transfection of mammalian cell lines, have established that the repetitive 38-amino acid repeat units represent a novel microtubule-binding motif. This motif is very similar in length to those of the mammalian microtubule-associated proteins Tau, MAP2, and MAP-U, but both its sequence and charge are different. The observation that the microtubule-binding motifs both of the neural and the trypanosomal proteins are of similar length may reflect the fact that both mediate binding to the same repetitive surface, the microtubule, while their sequence and charge differences are in agreement with the observation that they interact with different domains of the tubulins.

摘要

寄生性血鞭毛虫布氏锥虫细胞骨架的主要成分是膜骨架,它由单层紧密排列的微管组成。这一微管阵列包围着整个细胞体,并与覆盖其上的细胞膜相邻且相连。该阵列中的微管含有众多微管相关蛋白。其中最突出的是一个高分子量的重复蛋白家族,它们在很大程度上由串联排列的38个氨基酸的重复单元组成。现在已经在体外和体内对这些蛋白之一的MARP-1与微管的结合进行了表征。MARP-1通过微管蛋白结构域与微管结合,而不是通过哺乳动物脑微管相关蛋白(如MAP2或Tau)所使用的COOH末端。使用重组蛋白的体外结合试验以及哺乳动物细胞系的转染表明,38个氨基酸的重复单元代表一种新的微管结合基序。该基序的长度与哺乳动物微管相关蛋白Tau、MAP2和MAP-U的基序非常相似,但其序列和电荷不同。神经蛋白和锥虫蛋白的微管结合基序长度相似这一观察结果可能反映了这样一个事实,即两者都介导与同一重复表面微管的结合,而它们的序列和电荷差异与它们与微管蛋白不同结构域相互作用的观察结果一致。

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本文引用的文献

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The Cytoskeleton of trypanosomes.
Parasitol Today. 1990 Feb;6(2):49-52. doi: 10.1016/0169-4758(90)90069-g.
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Developmental cycles and biology of pathogenic trypanosomes.致病性锥虫的发育周期与生物学特性
Br Med Bull. 1985 Apr;41(2):105-14. doi: 10.1093/oxfordjournals.bmb.a072036.

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