Bahraoui E, Clerget-Raslain B, Chapuis F, Olivier R, Parravicini C, Yagello M, Montagnier L, Gluckman J C
Unité d'Oncologie Virale, Institut Pasteur, Paris, France.
AIDS. 1988 Jun;2(3):165-9.
We have investigated the possible involvement in the interaction between HIV gp110 and its CD4 receptor of epitopes different from the currently known binding site(s) of the molecule. Four monoclonal antibodies (MAbs) to gp110 were used (Genetic Systems Corporation, Seattle, Washington, USA): one (110-1) recognized a peptide corresponding to the C-terminal part of gp110 (494-517); the other three (110-3, 110-4, 110-5) recognized the same peptide located at position 308-328. HIV or purified gp110 obtained from a vaccinia recombinant (Transgene S.A., Strasbourg, France) were pre-incubated with the MAb prior to addition to CD4+ cells. Specific binding of viral particles or of the soluble molecule was then determined by flow cytometer analysis, compared with that of control preparations where the MAb was added after HIV or gp 110 had been allowed to bind CD4+ cells. Significant inhibition of HIV binding was noted with the three MAbs to peptide (308-328), but not with 110-1. At the molecular level, these same MAbs decreased the affinity of interaction between CD4 and soluble gp110, although they could still label the latter molecule after it had bound to CD4+ cells. Therefore, steric hindrance may account for neutralization of HIV binding by antibodies that are actually directed to epitopes topographically distinct from the site of binding of gp110 to CD4.
我们研究了与HIV gp110及其CD4受体相互作用相关的可能性,这些表位不同于该分子目前已知的结合位点。使用了四种针对gp110的单克隆抗体(MAb)(美国华盛顿州西雅图市的遗传系统公司):一种(110-1)识别对应于gp110 C末端部分的肽段(494-517);另外三种(110-3、110-4、110-5)识别位于308-328位的相同肽段。在加入CD4+细胞之前,先将HIV或从痘苗重组体(法国斯特拉斯堡的Transgene S.A.公司)获得的纯化gp110与单克隆抗体预孵育。然后通过流式细胞仪分析确定病毒颗粒或可溶性分子的特异性结合,并与在HIV或gp110已经与CD4+细胞结合后再加入单克隆抗体的对照制剂进行比较。针对肽段(308-328)的三种单克隆抗体可显著抑制HIV的结合,但110-1则无此作用。在分子水平上,同样是这些单克隆抗体降低了CD4与可溶性gp110之间相互作用的亲和力,尽管在gp110与CD4+细胞结合后它们仍能标记该分子。因此,空间位阻可能是实际上针对与gp110结合CD4位点在拓扑结构上不同的表位的抗体中和HIV结合的原因。
