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微管蛋白-秋水仙碱复合物对微管动态不稳定性的影响。

Effects of the tubulin-colchicine complex on microtubule dynamic instability.

作者信息

Vandecandelaere A, Martin S R, Schilstra M J, Bayley P M

机构信息

Division of Physical Biochemistry, National Institute for Medical Research, Mill Hill, London, U.K.

出版信息

Biochemistry. 1994 Mar 15;33(10):2792-801. doi: 10.1021/bi00176a007.

Abstract

The effects of the tubulin-colchicine complex (Tu-Col) on the dynamic behavior of microtubules have been examined under steady-state conditions in vitro. The addition of Tu-Col to tubulin microtubules at steady state results in only partial microtubule disassembly. Nevertheless, both the rate and the extent of tubulin exchange into microtubules are markedly suppressed by concentrations of Tu-Col which are low relative to the total amount of free tubulin. In addition, the time-dependent changes in microtubule length distribution, characteristic of dynamic instability, are suppressed by the addition of Tu-Col. Examination by video-enhanced dark-field microscopy of individual microtubules in the presence of Tu-Col shows that the principal effect of this complex is to reduce the growth rate at both ends of the microtubule. We have used computer simulation to rationalize the action of Tu-Col in terms of its effects on the experimentally observable parameters, namely, the rates of growth and shortening and the mean lifetimes of growth and shortening, which provide an empirical description of the dynamic behavior of microtubules. The results have been interpreted within the framework of the lateral cap formulation for microtubule dynamic instability [Martin, S. R., Schilstra, M. J., & Bayley, P. M. (1993) Biophys. J. 65, 578-596]. The simplest model mechanism requires only that Tu-Col binds to the microtubule end and inhibits further addition reactions in either the 5-start or the 8-start direction of the microtubule lattice. Monte Carlo simulations show that Tu-Col can, in this way, cause major suppression of the dynamic transitions of microtubules without inducing bulk microtubule disassembly. This type of mechanism could be important for the regulation of microtubule dynamics in vivo.

摘要

在体外稳态条件下,已对微管蛋白 - 秋水仙碱复合物(Tu - Col)对微管动态行为的影响进行了研究。在稳态下向微管蛋白微管中添加Tu - Col只会导致部分微管解聚。然而,相对于游离微管蛋白的总量而言,低浓度的Tu - Col就能显著抑制微管蛋白向微管中交换的速率和程度。此外,添加Tu - Col可抑制微管长度分布随时间的变化,这种变化是动态不稳定性的特征。通过视频增强暗场显微镜观察在Tu - Col存在下的单个微管表明,该复合物的主要作用是降低微管两端的生长速率。我们已使用计算机模拟,根据Tu - Col对实验可观察参数的影响来解释其作用,这些参数即生长和缩短的速率以及生长和缩短的平均寿命,它们提供了对微管动态行为的经验性描述。结果已在微管动态不稳定性的侧帽模型框架内进行了解释[Martin, S. R., Schilstra, M. J., & Bayley, P. M. (1993) Biophys. J. 65, 578 - 596]。最简单的模型机制仅要求Tu - Col结合到微管末端,并抑制微管晶格在5起始或8起始方向上的进一步添加反应。蒙特卡罗模拟表明,Tu - Col可以通过这种方式导致微管动态转变的主要抑制,而不会诱导大量微管解聚。这种机制类型对于体内微管动力学的调节可能很重要。

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