Prusoff W, Lin T S, Pivazyan A, Sun A S, Birks E
Department of Pharmacology, Yale University, New Haven, CT 06510.
Pharmacol Ther. 1993 Nov;60(2):315-29. doi: 10.1016/0163-7258(93)90013-4.
The human immunodeficiency virus, HIV-1, is generally accepted to be responsible for AIDS. It is imperative that all approaches, empirical and rational, be taken for development of a drug for therapy of this disease. These approaches are discussed, with emphasis on the direction being pursued in our laboratory. Empirically, we found 3'-deoxy-2',3'-didehydrothymidine, a compound first synthesized for potential anticancer activity by J. Horwitz in the 1960s, to be a potent inhibitor of HIV-1. It is now in Phase II/III clinical trials. We have also synthesized several 2,5'-anhydro pyrimidine nucleoside analogs, which have interesting chemical and biological properties. We have evaluated a natural product, gossypol and synthesized various derivatives for anti-HIV-1 activity, but none were appreciably more inhibitory than the parent compound. More recently, we have taken the rational approach and synthesized a boron-modified tetrapeptide, Ac-Thr-Leu-Asn-boro-Phe, which corresponds to the COOH-terminal of the Phe-Pro scissle bond of the gag/pol gene polyprotein product. Potent inhibition of the HIV-1 encoded protease was observed. These approaches and findings will be discussed.
人类免疫缺陷病毒1型(HIV-1)被普遍认为是导致艾滋病的病原体。开发治疗该疾病的药物时,必须采用所有经验性和理性的方法。本文将讨论这些方法,并重点介绍我们实验室正在探索的方向。从经验角度来看,我们发现3'-脱氧-2',3'-双脱氢胸苷(一种20世纪60年代由J. Horwitz首次合成用于潜在抗癌活性的化合物)是HIV-1的有效抑制剂。它目前正处于II/III期临床试验阶段。我们还合成了几种2,5'-脱水嘧啶核苷类似物,它们具有有趣的化学和生物学特性。我们评估了一种天然产物棉酚,并合成了各种衍生物用于抗HIV-1活性,但没有一种比母体化合物具有更明显的抑制作用。最近,我们采用了理性方法,合成了一种硼修饰的四肽Ac-Thr-Leu-Asn-boro-Phe,它对应于gag/pol基因多蛋白产物的Phe-Pro裂解键的COOH末端。观察到对HIV-1编码蛋白酶有强效抑制作用。将讨论这些方法和发现。
