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首页> 外文期刊>Bioorganic and Medicinal Chemistry Letters >Key analogs of a uniquely potent synthetic vinblastine that contain modifications of the C20' ethyl substituent
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Key analogs of a uniquely potent synthetic vinblastine that contain modifications of the C20' ethyl substituent

机译:含有C20'乙基取代基的改性的唯一有效合成式调温剂的关键类似物

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摘要

A key series of vinblastine analogs 7-13, which contain modifications to the C20' ethyl group, was prepared with use of two distinct synthetic approaches that provide modifications of the C20' side chain containing linear and cyclized alkyl groups or added functionalized substituents. Their examination revealed the unique nature of the improved properties of the synthetic vinblastine 6, offers insights into the origins of its increased tubulin binding affinity and 10-fold improved cell growth inhibition potency, and served to probe a small hydrophobic pocket anchoring the binding of vinblastine with tubulin. Especially noteworthy were the trends observed with substitution of the terminal carbon of the ethyl group that, with the exception of 9 (R = F vs H, equipotent), led to remarkably substantial reductions in activity (>10-fold): R = F (equipotent with H)> N3, CN (10-fold) > Me (50-fold) > Et (100-fold) > OH (inactive). This is in sharp contrast to the maintained (7) or enhanced activity (6) observed with its incorporation into a cyclic C20'/C15'-fused six-membered ring. (C) 2017 Elsevier Ltd. All rights reserved.
机译:使用两种不同的合成方法使用两种不同的合成方法制备含有对C20'乙基的修饰的长春碱类似物7-13系列的键系列的键系列含有对C20'乙基的修饰。提供含有线性和环化烷基的C20'侧链或加入官能化取代基的修饰。他们的检查揭示了合成式长春碱6的改善性质的独特性,提供了进入其增加的小管蛋白结合亲和力和10倍改善的细胞生长抑制效力的洞察力,并用于探测锚固锚固的小疏水口袋用管蛋白。特别值得注意的是替代乙基末端碳的趋势,除了9(r = f Vs H,等待电偶),LED可显着降低活动(> 10倍):r = f (使用H)> N 3,CN(10倍)> ME(50倍)>等(100倍)> OH(无效)。这与通过掺入环状C20' / C15'-熔融的六元环观察到的维持(7)或增强的活性(6)呈鲜明对比。 (c)2017 Elsevier Ltd.保留所有权利。

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