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HIV-1 Gag as an Antiviral Target: Development of Assembly and Maturation Inhibitors

机译:HIV-1堵嘴作为一种抗病毒目标:装配和成熟抑制剂的发展。

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摘要

HIV-1 Gag is the master orchestrator of particle assembly. The central role of Gag at multiple stages of the HIV lifecycle has led to efforts to develop drugs that directly target Gag and prevent the formation and release of infectious particles. Until recently, however, only the catalytic site protease inhibitors have been available to inhibit late stages of HIV replication. This review summarizes the current state of development of antivirals that target Gag or disrupt late events in the retrovirus lifecycle such as maturation of the viral capsid. Maturation inhibitors represent an exciting new series of antiviral compounds, including those that specifically target CA-SP1 cleavage and the allosteric integrase inhibitors that inhibit maturation by a completely different mechanism. Numerous small molecules and peptides targeting CA have been studied in attempts to disrupt steps in assembly. Efforts to target CA have recently gained considerable momentum from the development of small molecules that bind CA and alter capsid stability at the post-entry stage of the lifecycle. Efforts to develop antivirals that inhibit incorporation of genomic RNA or to inhibit late budding events remain in preliminary stages of development. Overall, the development of novel antivirals targeting Gag and the late stages in HIV replication appears much closer to success than ever, with the new maturation inhibitors leading the way.
机译:HIV-1 Gag是粒子装配的主要协调者。 Gag在HIV生命周期的多个阶段的核心作用导致人们致力于开发直接针对Gag并防止感染性颗粒形成和释放的药物。然而,直到最近,仅催化位点蛋白酶抑制剂可用于抑制HIV复制的后期。这篇综述总结了靶向Gag或破坏逆转录病毒生命周期中的晚期事件(例如病毒衣壳的成熟)的抗病毒药物的当前开发状态​​。成熟抑制剂代表了一系列激动人心的抗病毒化合物,包括专门针对CA-SP1裂解的化合物和通过完全不同的机制抑制成熟的变构整合酶抑制剂。已经研究了许多靶向CA的小分子和肽,试图破坏组装步骤。由于在生命周期的进入后阶段结合CA并改变衣壳稳定性的小分子的发展,针对CA的努力最近获得了可观的动力。开发抑制基因组RNA掺入或抑制后期出芽事件的抗病毒药物的努力仍处于开发的初期阶段。总体而言,以新的成熟抑制剂为主导,开发针对Gag的新型抗病毒药物和HIV复制的后期阶段似乎比以往更接近成功。

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