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Debio-025 通过干扰 HIV-1 复制周期中的早期事件来抑制 HIV-1。

Debio-025 inhibits HIV-1 by interfering with an early event in the replication cycle.

机构信息

Rega Institute for Medical Research, Katholieke Universiteit Leuven, Minderbroedersstraat 10, B-3000 Leuven, Belgium.

出版信息

Antiviral Res. 2010 Feb;85(2):418-21. doi: 10.1016/j.antiviral.2009.10.009. Epub 2009 Oct 24.

Abstract

Cyclophilin A is a peptidyl-propyl isomerase that binds the capsid (p24) protein of HIV-1 and facilitates replication. We report a cyclophilin inhibitor, a non-immunosuppressive cyclosporine analogue, Debio-025, that is about 15-times more potent than cyclosporine A and less toxic resulting in a selectivity index of more than 300. It was equally active against virus strains that were resistant toward inhibitors of the viral entry, fusion, or reverse transcription while it was not inhibitory to HIV-2 or SIV(MAC). Mechanism of action studies demonstrate that Debio-025 inhibits the HIV-1 replication by interfering with an early stage of the viral replication cycle. Indeed, addition of Debio-025 could be postponed for 2h before loosing its antiviral activity. The compound proved inactive against mutant viruses that are independent of cyclophilin A binding suggesting Debio-025 targets the cyclophilin A-capsid interaction.

摘要

亲环素 A 是一种肽基丙氨酸异构酶,可结合 HIV-1 的衣壳(p24)蛋白并促进复制。我们报告了一种亲环素抑制剂,即非免疫抑制剂环孢素类似物 Debio-025,其效力比环孢素 A 高约 15 倍,毒性更低,因此选择性指数超过 300。它对抵抗病毒进入、融合或逆转录抑制剂的病毒株同样有效,而对 HIV-2 或 SIV(MAC)没有抑制作用。作用机制研究表明,Debio-025 通过干扰病毒复制周期的早期阶段来抑制 HIV-1 的复制。事实上,在失去抗病毒活性之前,添加 Debio-025 可以推迟 2 小时。该化合物对不依赖亲环素 A 结合的突变病毒无效,表明 Debio-025 靶向亲环素 A-衣壳相互作用。

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