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Evaluation of CD4-CD4i Antibody Architectures Yields Potent Broadly Cross-Reactive Anti-Human Immunodeficiency Virus Reagents

机译:CD4-CD4i抗体体系结构的评估产生有效的广泛交叉反应的抗人类免疫缺陷病毒试剂

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摘要

The envelope glycoprotein of human immunodeficiency virus type 1 (HIV-1) has several adaptations that allow the virus to evade antibody neutralization. Nevertheless, a few broadly cross-reactive neutralizing antibodies as well as reagents containing portions of CD4, the HIV receptor, have demonstrated partial efficacy in suppressing viral replication. One type of reagent designed for improved HIV neutralization fuses the CD4 D1-D2 domains to the variable regions of an antibody recognizing the CD4-induced (CD4i) coreceptor binding site on the gp120 portion of the HIV envelope spike. We designed, expressed, purified, and tested the neutralization potencies of CD4-CD4i antibody reagents with different architectures, antibody combining sites, and linkers. We found that fusing CD4 to the heavy chain of the CD4i antibody E51 yields a bivalent reagent including an antibody Fc region that expresses well, is expected to have a long serum half-life, and has comparable or greater neutralization activity than well-known broadly neutralizing anti-HIV antibodies. A CD4 fusion with the anti-HIV carbohydrate antibody 2G12 also results in a potent neutralizing reagent with more broadly neutralizing activity than 2G12 alone.
机译:1型人类免疫缺陷病毒(HIV-1)的包膜糖蛋白具有多种适应性,可让该病毒逃避抗体中和。然而,一些广泛的交叉反应中和抗体以及含有CD4部分(HIV受体)的试剂已显示出抑制病毒复制的部分功效。设计用于改善HIV中和的一种类型的试剂将CD4 D1-D2结构域融合到抗体的可变区,该抗体识别HIV包膜刺突gp120部分上的CD4诱导的(CD4i)共受体结合位点。我们设计,表达,纯化和测试了具有不同结构,抗体结合位点和接头的CD4-CD4i抗体试剂的中和潜能。我们发现,将CD4融合到CD4i抗体E51的重链上会产生一种二价试剂,该抗体包括表达良好的Fc区,预期具有较长的血清半衰期,并且具有与广为人知的抗体相当或更高的中和活性中和抗HIV抗体。 CD4与抗HIV碳水化合物抗体2G12的融合还产生了比单独的2G12更广泛的中和活性的有效中和试剂。

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