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Design, synthesis, and evaluation of 3C protease inhibitors as anti-enterovirus 71 agents.

机译:设计,合成和评估3C蛋白酶抑制剂作为抗肠道病毒71剂。

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摘要

Human enterovirus (EV) belongs to the picornavirus family, which consists of over 200 medically relevant viruses. A peptidomimetic inhibitor AG7088 was developed to inhibit the 3C protease of rhinovirus (a member of the family), a chymotrypsin-like protease required for viral replication, by forming a covalent bond with the active site Cys residue. In this study, we have prepared the recombinant 3C protease from EV71 (TW/2231/98), a particular strain which causes severe outbreaks in Asia, and developed inhibitors against the protease and the viral replication. For inhibitor design, the P3 group of AG7088, which is not interacting with the rhinovirus protease, was replaced with a series of cinnamoyl derivatives directly linked to P2 group through an amide bond to simplify the synthesis. While the replacement caused decreased potency, the activity can be largely improved by substituting the alpha,beta-unsaturated ester with an aldehyde at the P1' position. The best inhibitor 10b showed EC(50) of 18 nM without apparent toxicity (CC(50)>25 microM). Our study provides potent inhibitors of the EV71 3C protease as anti-EV71 agents and facilitates the combinatorial synthesis of derivatives for further improving the inhibitory activity.
机译:人肠道病毒(EV)属于小核糖核酸病毒家族,由200多种医学上相关的病毒组成。拟肽抑制剂AG7088通过与活性位点Cys残基形成共价键来抑制鼻病毒(家族成员)的3C蛋白酶,这是一种病毒复制所需的胰凝乳蛋白酶样蛋白酶。在这项研究中,我们从EV71(TW / 2231/98)制备了重组3C蛋白酶,EV71是在亚洲引起严重疫情的特殊菌株,并开发了针对蛋白酶和病毒复制的抑制剂。为了进行抑制剂设计,将不与鼻病毒蛋白酶相互作用的AG7088的P3基团替换为通过酰胺键直接连接到P2基团的一系列肉桂酰基衍生物,以简化合成。虽然替代导致效力降低,但是可以通过在P1'位置用醛取代α,β-不饱和酯来大大提高活性。最佳抑制剂10b的EC(50)为18 nM,无明显毒性(CC(50)> 25 microM)。我们的研究提供了有效的EV71 3C蛋白酶抑制剂作为抗EV71剂,并促进了衍生物的组合合成,从而进一步提高了抑制活性。

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