Cavacini L A, Emes C L, Power J, Underdahl J, Goldstein R, Mayer K, Posner M R
Department of Medicine, New England Deaconess Hospital, Boston, MA 02215.
J Acquir Immune Defic Syndr (1988). 1993 Oct;6(10):1093-102.
Serum antibody reactive with epitopes within the CD4 binding site (CD4BS) of HIV-1/gp120 on infected cells was measured by inhibition of binding of a human monoclonal antibody, F105, which recognizes a conformational epitope within this region. Serum samples from 27% of ARC/AIDS patients blocked binding of F105 to this epitope, while samples from 100% of asymptomatic seropositive patients blocked binding. F105 blocking activity increased in 87% of asymptomatic donors who maintained stable disease over a 3-6 year period and decreased in 50% of asymptomatic patients with progressive disease. Moreover, serum samples from patients with stable disease exhibited higher titers of F105 blocking activity. The presence of F105 blocking activity also correlated with serum neutralization of virus. When diluted 1:640, serum with low F105 blocking activity neutralized only 20-30% of viral cytopathic effect (CPE), while serum with high F105 blocking activity neutralized > 80%. Serum neutralization was enhanced by the addition of F105. Seroreactivity to infected cells was detectable within 6 months of seroconversion, but F105 blocking activity was delayed by an additional 6-12 months, as was the development of high titers of neutralizing antibody. These data support the notion that the humoral response to the CD4BS on gp120 may be important in the maintenance of health.
通过抑制人单克隆抗体F105的结合来测量感染细胞上与HIV-1/gp120的CD4结合位点(CD4BS)内表位发生反应的血清抗体,F105可识别该区域内的一个构象表位。27%的艾滋病相关综合征/艾滋病患者的血清样本可阻断F105与该表位的结合,而100%无症状血清阳性患者的样本可阻断结合。在3至6年期间病情保持稳定的无症状供者中,87%的人F105阻断活性增强,而病情进展的无症状患者中有50%的人F105阻断活性降低。此外,病情稳定的患者的血清样本表现出更高的F105阻断活性滴度。F105阻断活性的存在也与血清对病毒的中和作用相关。当稀释至1:640时,F105阻断活性低的血清仅中和20%-30%的病毒细胞病变效应(CPE),而F105阻断活性高的血清中和率>80%。添加F105可增强血清中和作用。血清转化后6个月内可检测到对感染细胞的血清反应性,但F105阻断活性会额外延迟6至12个月出现,高滴度中和抗体的产生也是如此。这些数据支持这样一种观点,即针对gp120上CD4BS的体液反应可能对维持健康很重要。
