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三磷酸腺苷(ATP)对微管组装动力学的影响。

Effect of ATP on the kinetics of microtubule assembly.

作者信息

Zabrecky J R, Cole R D

出版信息

J Biol Chem. 1982 Apr 25;257(8):4633-8.

PMID:7068656
Abstract

We investigated the role of ATP in the assembly of microtubules. Tubulin, prepared by chromatography on DEAE-cellulose, was nearly devoid of nucleoside diphosphokinase activity. ATP induced assembly in such preparations for a single assembly/disassembly cycle; then further assembly could not be induced by ATP unless the system was supplemented with additional GTP. This suggests that the E-site must contain GTP for polymerization and ATP interacts at a different site on tubulin. Although tubulin can be assembled into microtubules in 1.0 mM GTP, the inclusion of 0.2 mM ATP along with the GTP increases the rate and extent of assembly. The enhancement increased with increasing ATP concentrations. The inclusion of 0.2 mM ATP reduced the critical concentration for tubulin assembly from 1.5 to 0.9 mg/ml. Analysis of assembly rate versus protein concentration suggested that ATP also affects nucleation. Aggregates of tubulin rings formed by warming tubulin in the presence of 1.0 mM ATP and 5.0 mM Mg2+ were capable of initiating assembly in a solution of tubulin which was not able to polymerize. Furthermore, the extent of microtubule formation was dependent on the concentration of aggregated rings added to the solution. We propose that ATP interacts with tubulin at a binding site that is distinct from the N- and E-sites that bind GTP. A function of ATP binding is to stimulate the formation of tubulin rings as nucleation centers for polymerization.

摘要

我们研究了ATP在微管组装中的作用。通过在DEAE - 纤维素上进行色谱法制备的微管蛋白几乎没有核苷二磷酸激酶活性。ATP在这样的制剂中诱导单个组装/拆卸循环的组装;然后除非系统补充额外的GTP,否则ATP不能诱导进一步的组装。这表明E位点必须含有GTP才能进行聚合,并且ATP在微管蛋白的不同位点相互作用。虽然微管蛋白可以在1.0 mM GTP中组装成微管,但将0.2 mM ATP与GTP一起加入会增加组装的速率和程度。随着ATP浓度的增加,这种增强作用也增加。加入0.2 mM ATP将微管蛋白组装的临界浓度从1.5降至0.9 mg/ml。组装速率与蛋白质浓度的分析表明ATP也影响成核。在1.0 mM ATP和5.0 mM Mg2+存在下加热微管蛋白形成的微管蛋白环聚集体能够在不能聚合的微管蛋白溶液中引发组装。此外,微管形成的程度取决于添加到溶液中的聚集环的浓度。我们提出ATP在一个与结合GTP的N位点和E位点不同的结合位点与微管蛋白相互作用。ATP结合的一个功能是刺激微管蛋白环的形成作为聚合的成核中心。

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