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微管蛋白与大分子非极性探针辛基琼脂糖的相互作用。

Interaction of tubulin with the macromolecular apolar probe, octyl sepharose.

作者信息

Prasad A R, Prasad V, Ludueña R F, Horowitz P M

出版信息

Biochem Biophys Res Commun. 1987 Jun 15;145(2):949-55. doi: 10.1016/0006-291x(87)91057-6.

Abstract

Binding of the microtubule protein, tubulin, to hydrophobic groups immobilized on octyl sepharose has been investigated. The results indicate that tubulin binds to octyl sepharose in a time-, temperature-, and concentration-dependent manner. Binding is multiphasic, with one fast phase and at least two slow phases, and is influenced by the presence of antimitotic drugs. Colchicine, vinblastine and podophyllotoxin enhance the fast binding of tubulin with very little effect on the slow binding. Pre-incubation of tubulin with the apolar probe, bis(1,8-anilinonaphthalenesulfonate) (BisANS) enhances both the rapid and slow phases of binding of tubulin to octyl sepharose. 1,8-Anilinonaphthalenesulfonate, the monomer of BisANS, has no effect. These results are consistent with a model for tubulin decay which involves the appearance of hydrophobic sites with time.

摘要

对微管蛋白(微管素)与固定在辛基琼脂糖上的疏水基团的结合进行了研究。结果表明,微管素以时间、温度和浓度依赖性方式与辛基琼脂糖结合。结合是多相的,有一个快速相和至少两个缓慢相,并且受抗有丝分裂药物的存在影响。秋水仙碱、长春碱和鬼臼毒素增强了微管素的快速结合,对缓慢结合影响很小。微管素与非极性探针双(1,8-苯胺基萘磺酸盐)(BisANS)预孵育增强了微管素与辛基琼脂糖结合的快速相和缓慢相。BisANS的单体1,8-苯胺基萘磺酸盐没有影响。这些结果与一个涉及疏水位点随时间出现的微管素衰变模型一致。

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