Nehete P N, Arlinghaus R B, Sastry K J
Department of Molecular Pathology, University of Texas M. D. Anderson Cancer Center, Houston 77030.
J Virol. 1993 Nov;67(11):6841-6. doi: 10.1128/JVI.67.11.6841-6846.1993.
Because V3 loop-specific antibodies have been shown to inhibit human immunodeficiency virus type 1 (HIV-1) infection of human cells and because specific mutations in the V3 loop render the virus ineffective for infection and syncytium formation, we tested the anti-HIV effects of V3 loop peptides from different HIV-1 strains. We obtained evidence that V3 loop synthetic peptides of 8 to 15 amino acids at nanogram concentrations efficiently blocked HIV-1 IIIB infection of several human T-cell lines and of freshly prepared normal human T cells. More importantly, syncytium formation by three different primary clinical HIV isolates was inhibited by the V3 loop peptide from HIV-1 IIIB at a concentration of 1 micrograms/ml. Concentrations of V3 peptides up to 50 micrograms/ml were not toxic to any of the human cells studied. Additionally, V3 peptides incubated in normal human serum or plasma exhibited biological and physical stability for up to 24 h. Taken together, these results suggest that the V3 loop peptides have medical utility as therapeutic reagents to either prevent HIV-1 infection in humans or reduce the spread of virus infection in HIV-infected individuals. These findings are especially significant because a number of reports in the literature indicate that the V3 loop region in gp120 plays an important role in the initial stages of HIV-1 infection of cells.
由于V3环特异性抗体已被证明可抑制人类免疫缺陷病毒1型(HIV-1)对人类细胞的感染,并且由于V3环中的特定突变会使病毒无法有效感染和形成合胞体,我们测试了来自不同HIV-1毒株的V3环肽的抗HIV作用。我们获得的证据表明,纳克浓度的8至15个氨基酸的V3环合成肽可有效阻断几种人类T细胞系以及新鲜制备的正常人T细胞的HIV-1 IIIB感染。更重要的是,来自HIV-1 IIIB的V3环肽在浓度为1微克/毫升时可抑制三种不同的原发性临床HIV分离株形成合胞体。高达50微克/毫升的V3肽浓度对所研究的任何人类细胞均无毒。此外,在正常人血清或血浆中孵育的V3肽在长达24小时内表现出生物学和物理稳定性。综上所述,这些结果表明,V3环肽作为治疗试剂具有医学用途,可用于预防人类HIV-1感染或减少HIV感染者中病毒感染的传播。这些发现尤为重要,因为文献中的许多报告表明,gp120中的V3环区域在HIV-1感染细胞的初始阶段起着重要作用。
