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双(1,8-苯胺基萘磺酸盐)。一种新型且强效的微管组装抑制剂。

Bis(1,8-anilinonaphthalenesulfonate). A novel and potent inhibitor of microtubule assembly.

作者信息

Horowitz P, Prasad V, Luduena R F

出版信息

J Biol Chem. 1984 Dec 10;259(23):14647-50.

PMID:6548750
Abstract

Two related compounds, 1,8-anilinonaphthalenesulfonate (1,8-ANS) and bis(1,8-anilinonaphthalenesulfonate) (Bis-ANS), are useful fluorescent probes for hydrophobic areas on protein molecules. Using fluorescence, we examined the binding of these compounds to bovine brain tubulin and found that Bis-ANS and 1,8-ANS bound to tubulin with Ki values of 2 and 25 microM, respectively. Bis-ANS potently inhibited the polymerization of tubulin into microtubules in vitro. In the presence of microtubule-associated protein 2, half-maximal inhibition of assembly was obtained at 3 microM Bis-ANS. In the presence of tau protein, half-maximal inhibition was obtained at 15 microM Bis-ANS. Surprisingly, 1,8-ANS, even at 200 microM, did not inhibit assembly. Scatchard analysis indicated one binding site for Bis-ANS on tubulin. Previous reports of 1,8-ANS binding to tubulin may have been influenced by the presence of Bis-ANS which until recently was a common contaminant of commercial supplies. Because of its intense fluorescence in addition to its potent inhibitory effects, Bis-ANS appears to be a useful probe to study microtubule assembly and other interactions involving tubulin.

摘要

两种相关化合物,1,8 - 苯胺基萘磺酸盐(1,8 - ANS)和双(1,8 - 苯胺基萘磺酸盐)(Bis - ANS),是用于检测蛋白质分子疏水区域的有用荧光探针。利用荧光技术,我们检测了这些化合物与牛脑微管蛋白的结合情况,发现Bis - ANS和1,8 - ANS与微管蛋白结合的解离常数(Ki)值分别为2 microM和25 microM。Bis - ANS在体外能有效抑制微管蛋白聚合成微管。在微管相关蛋白2存在的情况下,3 microM的Bis - ANS可实现对微管组装的半数最大抑制。在tau蛋白存在的情况下,15 microM的Bis - ANS可实现半数最大抑制。令人惊讶的是,即使浓度达到200 microM,1,8 - ANS也不抑制微管组装。Scatchard分析表明Bis - ANS在微管蛋白上有一个结合位点。此前关于1,8 - ANS与微管蛋白结合的报道可能受到了Bis - ANS的影响,直到最近Bis - ANS仍是商业供应品中常见的污染物。由于其强烈的荧光以及强大的抑制作用,Bis - ANS似乎是研究微管组装及其他涉及微管蛋白的相互作用的有用探针。

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