Kaplan A H, Zack J A, Knigge M, Paul D A, Kempf D J, Norbeck D W, Swanstrom R
Department of Medicine, University of North Carolina, Chapel Hill 27599-7295.
J Virol. 1993 Jul;67(7):4050-5. doi: 10.1128/JVI.67.7.4050-4055.1993.
The production of infectious particles by human immunodeficiency virus type 1 is dependent on the accurate cleavage of its Gag and Gag/Pol precursors by a virally encoded protease. In the absence of protease activity, morphologically abnormal particles which are noninfectious are formed. Recently, inhibitors of the protease of human immunodeficiency virus type 1 have been developed as potential therapeutic agents. We have examined the basis for the loss of infectivity at the limiting inhibitor concentrations that are likely to be achieved in clinical settings. We found that subtle defects in processing are correlated with profound deficits in infectivity. Further, we correlated this partially disrupted processing with an altered virion morphology. These data suggest that accurate and complete processing is essential to the formation of infectious, morphologically normal virions and that the pathway by which these precursors are processed and assembled is sensitive to partial inhibition of the protease by an inhibitor disproportionate to the effect of the inhibitor on the viral protease itself.
1型人类免疫缺陷病毒感染性颗粒的产生依赖于病毒编码蛋白酶对其Gag和Gag/Pol前体的精确切割。在缺乏蛋白酶活性的情况下,会形成形态异常且无感染性的颗粒。最近,1型人类免疫缺陷病毒蛋白酶抑制剂已被开发为潜在的治疗药物。我们研究了在临床环境中可能达到的极限抑制剂浓度下感染性丧失的基础。我们发现加工过程中的细微缺陷与感染性的严重缺陷相关。此外,我们将这种部分中断的加工过程与病毒粒子形态的改变联系起来。这些数据表明,精确而完整的加工对于形成有感染性、形态正常的病毒粒子至关重要,并且这些前体的加工和组装途径对抑制剂对蛋白酶的部分抑制很敏感,这种抑制作用与抑制剂对病毒蛋白酶本身的作用不成比例。
