具有侧链的生物活性紫杉烷的合理设计。

Anti-cancer drug design Pub Date : 2000-02-01

J H Wu, L O Zamir

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引用次数: 0

摘要

对α -微管蛋白的结构进行了细化，并将其用于紫杉醇D、紫杉醇及其类似物的对接研究。用分子动力学方法研究了结合位点的构象空间。通过最小化β -微管蛋白活性位点计算相互作用能。杉杉素D中的C-5肉桂基侧链与紫杉醇的C-13侧链相似。具有新的C-5侧链的虚拟紫杉烷比紫杉杉素d具有更高的活性，如果改变核心骨架的构象，可以用新的C-5侧链取代C-13侧链。

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A rational design of bioactive taxanes with side chains situated elsewhere than on C-13.

The structure of alphabeta-tubulin was refined and used in the docking study for taxuspine D, paclitaxel and their analogues. The conformational space in the binding site was explored by molecular dynamics. The interaction energy was calculated by minimization in the active site of beta-tubulin. The C-5 cinnamoyl side chain in taxuspine D is found to mimic the C-13 side chain of paclitaxel. A virtual taxane with a new C-5 side chain is predicted to be more active than taxuspine D. The C-13 side chain could be replaced with a novel C-5 side chain if the conformation of the core skeleton is modified.

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Anti-cancer drug design

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