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Nonneutralizing Antibodies to the CD4-Binding Site on the gp120 Subunit of Human Immunodeficiency Virus Type 1 Do Not Interfere with the Activity of a Neutralizing Antibody against the Same Site

机译:人类免疫缺陷病毒1型gp120亚基CD4结合位点的非中和抗体不会干扰针对同一位点的中和抗体的活性。

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摘要

We have investigated whether nonneutralizing monoclonal antibodies (MAbs) to the gp120 subunit of the envelope glycoprotein (Env) complex of human immunodeficiency virus type 1 (HIV-1) can interfere with HIV-1 neutralization by another anti-gp120 MAb. We used neutralizing (b12) and nonneutralizing (205-42-15, 204-43-1, 205-46-9) MAbs to the epitope cluster overlapping the CD4-binding site (CD4BS) on gp120. All the MAbs, neutralizing or otherwise, cross-competed for binding to monomeric gp120, indicating the close topological proximity of their epitopes. However, the nonneutralizing CD4BS MAbs did not interfere with the neutralization activity of MAb b12. In contrast, in a binding assay using oligomeric Env expressed on the surface of Env-transfected cells, the nonneutralizing MAbs did partially compete with b12 for Env binding. The surface of Env-transfected cells contains two categories of binding site for CD4BS MAbs. One type of site is recognized by both b12 and nonneutralizing CD4BS MAbs; the other is recognized by only b12. Binding assays for Env-gp120 interactions based on the use of monomeric gp120 or Env-transfected cells do not predict the outcome of HIV-1 neutralization assays, and they should therefore be used only with caution when gauging the properties of anti-Env MAbs.
机译:我们已经研究了人类免疫缺陷病毒1型(HIV-1)包膜糖蛋白(Env)复合体gp120亚基的非中和性单克隆抗体(MAbs)是否可以通过另一种抗gp120 MAb干扰HIV-1中和。我们将中和(b12)和非中和(205-42-15、204-43-1、205-46-9)MAb用于重叠gp120上CD4结合位点(CD4BS)的表位簇。所有中和或其他形式的单克隆抗体交叉竞争以结合单体gp120,表明它们的表位在拓扑上紧密接近。但是,未中和的CD4BS MAb不会干扰MAb b12的中和活性。相反,在使用在Env转染的细胞表面表达的低聚Env的结合测定中,未中和的单克隆抗体确实与b12部分竞争Env结合。 Env转染的细胞表面包含CD4BS MAb的两类结合位点。 b12和非中和的CD4BS MAb均可识别一种类型的位点;另一个仅由b12识别。基于使用单体gp120或Env转染的细胞进行的Env-gp120相互作用的结合测定不能预测HIV-1中和测定的结果,因此在评估抗Env单抗的性质时应谨慎使用。

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