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引用本文:张建康,庄让笑,胡永洲.新型β-肽环氧酮类蛋白酶体抑制剂的合成与活性评价[J].中国现代应用药学,2015,32(11):1329-1336.
ZHANG Jiankang,ZHUANG Rangxiao,HU Yongzhou.Synthesis, Biological Evaluation of Novel β-Peptidyl Epoxyketone Proteasome Inhibitors[J].Chin J Mod Appl Pharm(中国现代应用药学),2015,32(11):1329-1336.
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新型β-肽环氧酮类蛋白酶体抑制剂的合成与活性评价
张建康1, 庄让笑1, 胡永洲2
1.杭州市西溪医院,杭州 310023;2.浙江大学药学院,杭州 310012
摘要:
目的 设计合成新型的β-肽类蛋白酶体抑制剂,并对其活性进行评价。方法 根据先导化合物Carfilzomib与蛋白酶体的作用方式,保留其与蛋白酶体结合的关键环氧酮片段,并结合β-氨基酸的特点,采用氨基酸替换、生物电子等排等药物设计的方法,设计一类结构新颖的蛋白酶体抑制剂;采用缩合、氧化、还原等反应,合成系列目标化合物;通过体外酶抑制活性实验检验化合物活性。结果 合成了8个结构新颖的β-肽环氧酮类衍生物,化合物结构经1H-NMR、ESI-MS确证,部分化合物体现了一定的蛋白酶体抑制活性。结论 β-氨基酸作为一种重要的α-氨基酸替换结构,有望能够丰富短肽类蛋白酶体抑制剂的结构类型。
关键词:  蛋白酶体抑制剂  β-肽环氧酮  合成  活性评价
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基金项目:
Synthesis, Biological Evaluation of Novel β-Peptidyl Epoxyketone Proteasome Inhibitors
ZHANG Jiankang1, ZHUANG Rangxiao1, HU Yongzhou2
1.Xixi Hospital of Hangzhou, Hangzhou 310023, China;2.College of Pharmaceutical Sciences, Zhejiang University, Hangzhou 310012, China
Abstract:
OBJECTIVE To discover novel β-peptidyl epoxyketone proteasome inhibitors, evaluate their enzymatic activities. METHODS According to the binding interactions of lead compound Carfilzomib with proteasome, the epoxyketone group of Carfilzomib was retained in the drug design. A series of novel proteasome inhibitors were designed by combining the retained epoxyketone group, β-amino acid using rational drug design strategies such as amino acid, bioisostere replacement. These compounds were synthesized through condensation, oxidation, reduction reactions, were tested for their enzymatic activities in vitro. RESULTS Totally 8 novel β-peptidyl epoxyketone analogues were synthesized, confirmed by 1H-NMR, ESI-MS, which exhibited moderate proteasome inhibitory activities. CONCLUSIONS β-Amino acid, which is an important α-amino acid replacement, is anticipated to enrich the structure diversity of proteasome inhibitors.
Key words:  proteasome inhibitors  β-peptidyl epoxyketone  synthesis  biological evaluation
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