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微管的刚性可通过稳定剂增强。

Rigidity of microtubules is increased by stabilizing agents.

作者信息

Mickey B, Howard J

机构信息

Department of Physiology and Biophysics, University of Washington, Seattle 98195-7290, USA.

出版信息

J Cell Biol. 1995 Aug;130(4):909-17. doi: 10.1083/jcb.130.4.909.

Abstract

Microtubules are rigid polymers that contribute to the static mechanical properties of cells. Because microtubules are dynamic structures whose polymerization is regulated during changes in cell shape, we have asked whether the mechanical properties of microtubules might also be modulated. We measured the flexural rigidity, or bending stiffness, of individual microtubules under a number of different conditions that affect the stability of microtubules against depolymerization. The flexural rigidity of microtubules polymerized with the slowly hydrolyzable nucleotide analogue guanylyl-(alpha, beta)-methylene-diphosphonate was 62 +/- 9 x 10(-24) Nm2 (weighted mean +/- SEM); that of microtubules stabilized with tau protein was 34 +/- 3 x 10(-24) Nm2; and that of microtubules stabilized with the antimitotic drug taxol was 32 +/- 2 x 10(-24) Nm2. For comparison, microtubules that were capped to prevent depolymerization, but were not otherwise stabilized, had a flexural rigidity of 26 +/- 2 x 10(-24) Nm2. Decreasing the temperature from 37 degrees C to approximately 25 degrees C, a condition that makes microtubules less stable, decreased the stiffness of taxol-stabilized microtubules by one-third. We thus find that the more stable a microtubule, the higher its flexural rigidity. This raises the possibility that microtubule rigidity may be regulated in vivo. In addition, the high rigidity of an unstabilized, GDP-containing microtubule suggests that a large amount of energy could be stored as mechanical strain energy in the protein lattice for subsequent force generation during microtubule depolymerization.

摘要

微管是一种刚性聚合物,对细胞的静态力学特性有贡献。由于微管是动态结构,其聚合在细胞形状变化过程中受到调控,我们不禁要问微管的力学特性是否也会受到调节。我们在多种不同条件下测量了单个微管的弯曲刚度(即抗弯刚度),这些条件会影响微管抗解聚的稳定性。用缓慢水解的核苷酸类似物鸟苷酰 -(α,β)-亚甲基二磷酸聚合的微管,其弯曲刚度为62±9×10⁻²⁴ N·m²(加权平均值±标准误);用微管相关蛋白tau稳定的微管,其弯曲刚度为34±3×10⁻²⁴ N·m²;用抗有丝分裂药物紫杉醇稳定的微管,其弯曲刚度为32±2×10⁻²⁴ N·m²。作为对照,经封端处理以防止解聚但未作其他稳定处理的微管,其弯曲刚度为26±2×10⁻²⁴ N·m²。将温度从37℃降至约25℃,这一条件会使微管稳定性降低,结果紫杉醇稳定的微管刚度降低了三分之一。因此我们发现,微管越稳定,其弯曲刚度越高。这就增加了微管刚度可能在体内受到调控的可能性。此外,未稳定的含GDP微管具有较高的刚度,这表明大量能量可能以机械应变能的形式存储在蛋白质晶格中,以便在微管解聚过程中随后产生力。

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