Kazmierski Wieslaw M, Kenakin Terry P, Gudmundsson Kristjan S
Division of Chemistry MV CEDD, GlaxoSmithKline, 5 Moore Drive, Research Triangle Park, NC 27709, USA.
Chem Biol Drug Des. 2006 Jan;67(1):13-26. doi: 10.1111/j.1747-0285.2005.00319.x.
This review highlights selected examples of peptide, peptidomimetic and small-molecule drug discovery targeting HIV-1 to advance novel anti-HIV pharmaceuticals that inhibit initial stages of the viral cycle; namely, attachment and entry. Some of these approaches have culminated in the development of peptide-based drugs, while other have exploited peptides as enabling tools toward the identification of small-molecule lead compounds. Both of these conceptually different approaches have facilitated lead optimization of molecules with complementary and often surprising anti-HIV pharmacological properties, supporting their role in pharmaceutical development. Furthermore, such molecules enabled mechanistic elucidation of viral attachment and entry and provided additional insights toward achieving the desired drug profile.
本综述重点介绍了针对人类免疫缺陷病毒1型(HIV-1)的肽、拟肽和小分子药物发现的精选实例,以推动新型抗HIV药物的研发,这些药物可抑制病毒周期的初始阶段,即附着和进入。其中一些方法最终促成了基于肽的药物的开发,而其他方法则利用肽作为识别小分子先导化合物的辅助工具。这两种概念上不同的方法都有助于对具有互补且往往令人惊讶的抗HIV药理特性的分子进行先导优化,支持它们在药物开发中的作用。此外,这类分子有助于从机制上阐明病毒的附着和进入,并为实现所需的药物特性提供了更多见解。
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