De Clercq E
Rega Institute for Medical Research, Katholieke Universiteit Leuven, Belgium.
Rev Med Virol. 2000 Jul-Aug;10(4):255-77. doi: 10.1002/1099-1654(200007/08)10:4<255::aid-rmv282>3.0.co;2-6.
Virtually all the compounds that are currently used, or under advanced clinical trial, for the treatment of HIV infections, belong to one of the following classes: (i) nucleoside/nucleotide reverse transcriptase inhibitors (NRTIs), (ii) non-nucleoside reverse transcriptase inhibitors (NNRTIs) and (iii) protease inhibitors (PIs). In addition to the reverse transcriptase and protease step, various other events in the HIV replicative cycle are potential targets for chemotherapeutic intervention: (i) viral adsorption, through binding to the viral envelope glycoprotein gp120 (polysulphates, polysulphonates, polyoxometalates, zintevir, negatively charged albumins); (ii) viral entry, through blockade of the viral coreceptors CXCR4 and CCR5 [bicyclams (AMD3100), polyphemusins (T22), TAK-779]; (iii) virus-cell fusion, through binding to the viral glycoprotein gp41 [T-20 (DP-178), siamycins, betulinic acid derivatives]; (iv) viral assembly and disassembly, through NCp7 zinc finger-targeted agents [2,2'-dithiobisbenzamides (DIBAs), azadicarbonamide (ADA)]; (v) proviral DNA integration, through integrase inhibitors such as L-chicoric acid; (vi) viral mRNA transcription, through inhibitors of the transcription (transactivation) process (peptoid CGP64222, fluoroquinolone K-12, Streptomyces product EM2487). Also, in recent years new NRTIs, NNRTIs and PIs have been developed that possess, respectively, improved metabolic characteristics (i.e. phosphoramidate and cyclosaligenyl pronucleotides of d4T), or increased activity against NNRTI-resistant HIV strains, or, in the case of PIs, a different, non-peptidic scaffold. Given the multitude of molecular targets with which anti-HIV agents can interact, one should be cautious in extrapolating from cell-free enzymatic assays to the mode of action of these agents in intact cells. A number of compounds (i.e. zintevir and L-chicoric acid, on the one hand; and CGP64222 on the other hand) have recently been found to interact with virus-cell binding and viral entry in contrast to their proposed modes of action targeted at the integrase and transactivation process, respectively.
目前用于治疗HIV感染或正处于高级临床试验阶段的几乎所有化合物都属于以下类别之一:(i)核苷/核苷酸逆转录酶抑制剂(NRTIs),(ii)非核苷逆转录酶抑制剂(NNRTIs)和(iii)蛋白酶抑制剂(PIs)。除了逆转录酶和蛋白酶步骤外,HIV复制周期中的各种其他事件也是化疗干预的潜在靶点:(i)病毒吸附,通过与病毒包膜糖蛋白gp120结合(多硫酸盐、聚磺酸盐、多金属氧酸盐、锌特韦、带负电荷的白蛋白);(ii)病毒进入,通过阻断病毒共受体CXCR4和CCR5 [双环胺类(AMD3100)、海螯虾抗菌肽(T22)、TAK - 779];(iii)病毒 - 细胞融合,通过与病毒糖蛋白gp41结合 [T - 20(DP - 178)、链霉菌素、桦木酸衍生物];(iv)病毒组装和拆卸,通过靶向NCp7锌指的药物 [2,2'-二硫代双苯甲酰胺(DIBAs)、氮杂二甲酰胺(ADA)];(v)前病毒DNA整合,通过整合酶抑制剂如L - 菊苣酸;(vi)病毒mRNA转录,通过转录(反式激活)过程的抑制剂(类肽CGP64222、氟喹诺酮K - 12、链霉菌产物EM2487)。此外,近年来还开发了新的NRTIs、NNRTIs和PIs,它们分别具有改善的代谢特性(即d4T的磷酰胺酸酯和环沙立基前体核苷酸),或对耐NNRTI的HIV毒株活性增加,或者就PIs而言,具有不同的非肽骨架。鉴于抗HIV药物可以相互作用的众多分子靶点,在从无细胞酶分析推断这些药物在完整细胞中的作用模式时应谨慎。最近发现一些化合物(一方面是锌特韦和L - 菊苣酸;另一方面是CGP64222)与病毒 - 细胞结合和病毒进入相互作用,这与它们分别针对整合酶和反式激活过程的拟议作用模式形成对比。
