HIV-1 capsid (CA) is an attractive target for its indispensable roles in the viral life cycle. We report the design, synthesis, and mechanistic study of a novel series of 2-piperazineone peptidomimetics as HIV capsid modulators by mimicking the structure of host factors binding to CA. F-Id-3o was the most potent compound from the synthesized series, with an anti-HIV-1 EC(50) value of 6.0 μM. However, this series of compounds showed a preference for HIV-2 inhibitory activity, in which Id-3o revealed an EC(50) value of 2.5 μM (anti-HIV-2 potency), an improvement over PF74. Interestingly, F-Id-3o did bind HIV-1 CA monomers and hexamers with comparable affinity, unlike PF74, consequently showing antiviral activity in the early and late stages of the HIV-1 lifecycle. Molecular dynamics simulations shed light on F-Id-3o and Id-3o binding modes within the HIV-1/2 CA protein and provide a possible explanation for the increased anti-HIV-2 potency. Metabolic stability assays in human plasma and human liver microsomes indicated that although F-Id-3o has enhanced metabolic stability over PF74, further optimization is necessary. Moreover, we utilized computational prediction of drug-like properties and metabolic stability of F-Id-3o and PF74, which correlated well with experimentally derived metabolic stability, providing an efficient computational pipeline for future preselection based on metabolic stability prediction. Overall, the 2-piperazineone-bearing peptidomimetics are a promising new chemotype in the CA modulators class with considerable optimization potential.
Design, synthesis, and mechanistic study of 2-piperazineone-bearing peptidomimetics as novel HIV capsid modulators.
2-哌嗪酮肽模拟物作为新型 HIV 衣壳调节剂的设计、合成和机理研究
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作者:Zhang Xujie, Sun Lin, Xu Shujing, Huang Tianguang, Zhao Fabao, Ding Dang, Liu Chuanfeng, Jiang Xiangyi, Tao Yucen, Kang Dongwei, De Clercq Erik, Pannecouque Christophe, Cocklin Simon, Dick Alexej, Liu Xinyong, Zhan Peng
| 期刊: | RSC Medicinal Chemistry | 影响因子: | 3.600 |
| 时间: | 2023 | 起止号: | 2023 Jun 2; 14(7):1272-1295 |
| doi: | 10.1039/d3md00134b | ||
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