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在碱性pH值下微管的组装与拆卸

Microtubule assembly and disassembly at alkaline pH.

作者信息

Regula C S, Pfeiffer J R, Berlin R D

出版信息

J Cell Biol. 1981 Apr;89(1):45-53. doi: 10.1083/jcb.89.1.45.

Abstract

Although it is now apparent that the intracellular pH may rise considerably above neutrality under physiological conditions, information on the effect of alkaline pH on microtubule assembly and disassembly is still quite fragmentay. We have studied the assembly/disassembly of bovine brain microtubule protein at alkaline pH in vitro. When microtubules are assembled to a new steady state at pH less than 7 and pH is then made more alkaline, they undergo a rapid disassembly to a new steady state. This disassembly is reversed by acidification. The degree of disassembly is determined largely by the pH- dependence of the critical concentration, which increases five to eight times, from pH 7 to 8. A fraction of assembly-incompetent tubulin is identified that increases with pH, but its incompetency is largely reversed with acidification. Measurements of microtubule lengths are used to indicate that disassembly occurs by uniform shortening of microtubules. A comparison of shortening by alkalinization with dilution suggests that the intrinsic rate of disassembly is accelerated by increasing pH. The capacity for initiating assembly is progressively lost with incubation at alkaline pH (although some protection is afforded by sulfhydryl-reducing agents). However, direct assembly from depolymerized mixtures is possible at least up to pH 8.3, and the steady state achieved at these alkaline pH values is stable. Such preparations are readily disassembled by cold and podophyllotoxin (PLN). Disassembly induced by PLN is also markedly enhanced at alkaline pH, suggesting a corresponding enhancement of "treadmilling." The implications of physiological events leading to alkaline shifts of pH for microtubule assembly/disassembly are discussed, particularly in the light of recent hypotheses regarding treadmilling and its role in controlling the distribution of microtubules in vivo.

摘要

尽管现在很明显,在生理条件下细胞内pH值可能会大幅上升至中性以上,但关于碱性pH值对微管组装和解聚影响的信息仍然相当零散。我们已经在体外研究了碱性pH值下牛脑微管蛋白的组装/解聚情况。当微管在pH值小于7的条件下组装到一个新的稳定状态,然后将pH值调至更碱性时,它们会迅速解聚到一个新的稳定状态。这种解聚通过酸化可以逆转。解聚的程度在很大程度上取决于临界浓度的pH依赖性,从pH 7到8,临界浓度会增加五到八倍。我们发现了一部分无组装能力的微管蛋白,其含量随pH值增加而增加,但其无能力状态在酸化后基本可以逆转。对微管长度的测量表明,解聚是通过微管均匀缩短发生的。将碱化导致的缩短与稀释导致的缩短进行比较表明,解聚的内在速率会随着pH值的升高而加快。在碱性pH值下孵育时,启动组装的能力会逐渐丧失(尽管巯基还原剂提供了一些保护)。然而,至少在pH 8.3之前,从解聚混合物中直接组装是可能的,并且在这些碱性pH值下达到的稳定状态是稳定的。这样的制剂很容易被低温和鬼臼毒素(PLN)解聚。在碱性pH值下,PLN诱导的解聚也会显著增强,这表明“踏车行为”相应增强。我们讨论了导致pH值碱性变化的生理事件对微管组装/解聚的影响,特别是鉴于最近关于踏车行为及其在体内控制微管分布作用的假说。

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