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微管蛋白-秋水仙碱复合物对微管的两端有着不同的毒害作用。

Tubulin-colchicine complexes differentially poison opposite microtubule ends.

作者信息

Farrell K W, Wilson L

出版信息

Biochemistry. 1984 Jul 31;23(16):3741-8. doi: 10.1021/bi00311a027.

Abstract

The kinetics of radiolabeled guanosine 5'-triphosphate-tubulin dimer addition to preformed microtubule copolymers, containing large numbers of tubulin-colchicine complexes (TCs), were examined at apparent equilibrium. The results indicated that radiolabeled dimer addition to copolymers occurs predominantly by a "treadmilling" reaction, analogous to that described for unpoisoned microtubules, and that some labeled dimer uptake also occurs by equilibrium exchange. The data further showed that TCs decrease the steady-state treadmilling reaction in a concentration-dependent manner. Since microtubule copolymers exhibited a treadmilling reaction, it was possible to differentially radiolabel opposite copolymer ends with [3H]- and [14C]guanine nucleotides and thus to measure the effects of TCs on dimer loss from opposite copolymer ends upon copolymer dilution. Dimer loss from both copolymer ends was inhibited in a concentration-dependent manner, but dimer loss from copolymer net assembly (A) ends (defined under steady-state conditions) was inhibited to a far greater extent than that from the opposite, net disassembly (D) copolymer ends. TCs therefore exhibited a graded, polar poisoning action, with copolymer A-end association and dissociation rate constants being far more susceptible to TC inhibition than those at the opposite copolymer D ends. The potential significance of this TC effect for regulating microtubule spatial orientation in vivo is discussed.

摘要

在表观平衡状态下,研究了放射性标记的鸟苷5'-三磷酸 - 微管蛋白二聚体添加到预先形成的微管共聚物中的动力学,该共聚物含有大量的微管蛋白 - 秋水仙碱复合物(TCs)。结果表明,放射性标记的二聚体添加到共聚物中主要通过“踏车运动”反应发生,类似于未中毒微管的情况,并且一些标记的二聚体摄取也通过平衡交换发生。数据进一步表明,TCs以浓度依赖性方式降低稳态踏车运动反应。由于微管共聚物表现出踏车运动反应,因此可以用[3H] - 和[14C]鸟嘌呤核苷酸对共聚物的相对两端进行差异放射性标记,从而测量TCs对共聚物稀释后相对两端二聚体损失的影响。共聚物两端的二聚体损失均以浓度依赖性方式受到抑制,但共聚物净组装(A)端(在稳态条件下定义)的二聚体损失受到的抑制程度远大于相对的净解聚(D)共聚物端。因此,TCs表现出分级的、极性中毒作用,共聚物A端的缔合和解离速率常数比共聚物相对的D端更容易受到TC抑制。讨论了这种TC效应在体内调节微管空间取向的潜在意义。

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