Design of coiled-coil N-peptides against HIV-1 based on a CADD strategy.

IF 2.9 3区化学 Q1 CHEMISTRY, ORGANIC

Organic & Biomolecular Chemistry Pub Date : 2024-11-11 DOI:10.1039/d4ob01620c

Yan Huang, Hui Luo, Yihui Jin, Yuheng Ma, Yan Zhao, Xin Gao, Yuting Zhao, Xiao Qi, Guodong Liang, Lu Ga, Gang Li, Jie Yang

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Abstract

Human Immunodeficiency Virus (HIV) has continued to endanger human health for decades and has a substantial impact on global health defence. Peptide-based fusion inhibitors, as an integral part of Highly Active Anti-Retroviral Therapy (HAART), are effective in preventing and controlling the AIDS epidemic. Nevertheless, the current market leader, Enfuvirtide, is facing numerous challenges in clinical application. We herein devised a cutting-edge development strategy leveraging SWISS-MODEL and HDOCK, enabling the design of artificial N-peptides. The most active compound, IZNP02QE, surpassed the positive control by demonstrating remarkable nanomolar-level inhibitory activity against HIV-1. Mechanistic investigations unveiled IZNP02QE's ability to disrupt the crucial endogenous 6-helix bundle (6-HB) by forming heteropolymers, underscoring its potential as a novel anti-HIV-1 agent. This work not only pioneers a novel design methodology for N-peptides but also opens up the possibility of a CADD strategy for designing peptide-based fusion inhibitors.

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基于 CADD 策略设计抗 HIV-1 的盘绕 N 肽。

几十年来，人类免疫缺陷病毒（HIV）一直危害着人类健康，并对全球卫生防护工作产生了重大影响。肽类融合抑制剂作为高活性抗逆转录病毒疗法（HAART）的重要组成部分，能够有效预防和控制艾滋病的流行。然而，目前市场上的领军药物恩夫韦肽在临床应用中面临着诸多挑战。在此，我们利用 SWISS-MODEL 和 HDOCK，设计出了最先进的人工 N 肽开发策略。活性最高的化合物 IZNP02QE 超越了阳性对照，对 HIV-1 具有显著的纳摩尔级抑制活性。机理研究揭示了 IZNP02QE 通过形成杂聚物破坏关键的内源性 6-螺旋束（6-HB）的能力，强调了其作为新型抗 HIV-1 药物的潜力。这项工作不仅开创了一种新的 N 肽设计方法，而且为设计基于肽的融合抑制剂的 CADD 策略提供了可能性。

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