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作为抗逆转录病毒药物的HIV-1衣壳抑制剂

HIV-1 Capsid Inhibitors as Antiretroviral Agents.

作者信息

Thenin-Houssier Suzie, Valente Susana T

机构信息

Department Immunology and Microbial Sciences, The Scripps Research Institute, 130 Scripps Way, 3C1, Jupiter, FL 33458, USA.

出版信息

Curr HIV Res. 2016;14(3):270-82. doi: 10.2174/1570162x14999160224103555.

Abstract

BACKGROUND

The infectious human immunodeficiency virus (HIV) particle is characterized by a conical capsid that encloses the viral RNA genome. The capsid is essential for HIV-1 replication and plays crucial roles in both early and late stages of the viral life cycle. Early on, upon fusion of the viral and cellular membranes, the viral capsid is released into the host cell cytoplasm and dissociates in a process known as uncoating, tightly associated with the reverse transcription of the viral genome. During the late stages of viral replication, the Gag polyprotein, precursor of the capsid protein, assemble at the plasma membrane to form immature non-infectious viral particles. After a maturation step by the viral protease, the capsid assembles to form a fullerene-like conical shape characteristic of the mature infectious particle. Mutations affecting the uncoating process, or capsid assembly and maturation, have been shown to hamper viral infectivity. The key role of capsid in viral replication and the absence of approved drugs against this protein have promoted the development of antiretrovirals. Screening based on the inhibition of capsid assembly and virtual screening for molecules binding to the capsid have successfully identified a number of potential small molecule compounds. Unfortunately, none of these molecules is currently used in the clinic.

CONCLUSION

Here we review the discovery and the mechanism of action of the small molecules and peptides identified as capsid inhibitors, and discuss their therapeutic potential.

摘要

背景

感染性人类免疫缺陷病毒(HIV)颗粒的特征是具有一个包裹病毒RNA基因组的锥形衣壳。衣壳对于HIV-1复制至关重要,并且在病毒生命周期的早期和晚期都发挥着关键作用。早期,在病毒膜与细胞膜融合后,病毒衣壳被释放到宿主细胞细胞质中,并在一个称为脱壳的过程中解离,这一过程与病毒基因组的逆转录紧密相关。在病毒复制的后期,衣壳蛋白的前体Gag多蛋白在质膜处组装形成不成熟的无感染性病毒颗粒。在病毒蛋白酶进行成熟步骤后,衣壳组装形成成熟感染性颗粒特有的类似富勒烯的锥形形状。已证明影响脱壳过程、衣壳组装和成熟的突变会阻碍病毒感染性。衣壳在病毒复制中的关键作用以及缺乏针对该蛋白的获批药物推动了抗逆转录病毒药物的研发。基于抑制衣壳组装的筛选以及针对与衣壳结合分子的虚拟筛选已成功鉴定出许多潜在的小分子化合物。不幸的是,目前这些分子均未用于临床。

结论

在此,我们综述了被鉴定为衣壳抑制剂的小分子和肽的发现及作用机制,并讨论了它们的治疗潜力。

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