首页> 美国卫生研究院文献>Journal of Virology >Immunization with a soluble CD4-gp120 complex preferentially induces neutralizing anti-human immunodeficiency virus type 1 antibodies directed to conformation-dependent epitopes of gp120.
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Immunization with a soluble CD4-gp120 complex preferentially induces neutralizing anti-human immunodeficiency virus type 1 antibodies directed to conformation-dependent epitopes of gp120.

机译:用可溶性CD4-gp120复合物免疫优先诱导针对gp120构象依赖性表位的中和性抗人免疫缺陷病毒1型抗体。

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摘要

Preservation of the conformation of recombinant gp120 in an adjuvant, enabling it to elicit conformation-dependent, epitope-specific, broadly neutralizing antibodies, may be critical for the development of any gp120-based human immunodeficiency virus type 1 (HIV-1) vaccine. It was hypothesized that recombinant gp120 complexed with recombinant CD4 could stabilize the conformation-dependent neutralizing epitopes and effectively deliver them to the immune system. Therefore, a soluble CD4-gp120 complex in Syntex adjuvant formulation was tested with mice for its ability to induce neutralizing anti-gp120 antibody responses. Seventeen monoclonal antibodies (MAbs) were generated and characterized. Immunochemical studies, neutralization assays, and mapping studies with gp120 mutants indicated that the 17 MAbs fell into three groups. Four of them were directed to what is probably a conformational epitope involving the C1 domain and did not possess virus-neutralizing activities. Another four MAbs bound to V3 peptide 302-321 and exhibited cross-reactive gp120 binding and relatively weak virus-neutralizing activities. These MAbs were very sensitive to amino acid substitutions, not only in the V3 regions but also in the base of the V1/V2 loop, implying a conformational constraint on the epitope. The last group of nine MAbs recognized conformation-dependent epitopes near the CD4 binding site of gp120 and inhibited the gp120-soluble CD4 interaction. Four of these nine MAbs showed broadly neutralizing activities against multiple laboratory-adapted strains of HIV-1, three of them neutralized only HIVIIIB, and the two lower-affinity MAbs did not neutralize any strain tested. Collectively, the results from this study indicate that immunization with the CD4-gp120 complex can elicit antibodies to conformationally sensitive gp120 epitopes, with some of the antibodies having broadly neutralizing activities. We suggest that immunization with CD4-gp120 complexes may be worth evaluating further for the development of an AIDS vaccine.
机译:在佐剂中保留重组gp120的构象,使其能够引发构象依赖性,表位特异性,广泛中和的抗体,对于开发任何基于gp120的1型人类免疫缺陷病毒(HIV-1)疫苗可能至关重要。据推测,与重组CD4复合的重组gp120可以稳定构象依赖性中和表位并将其有效地递送至免疫系统。因此,用小鼠测试了Syntex佐剂配方中的可溶性CD4-gp120复合物诱导中和性抗gp120抗体应答的能力。产生并表征了十七种单克隆抗体(MAb)。免疫化学研究,中和测定和gp120突变体的作图研究表明,这17个单抗分为3组。其中四个针对可能涉及C1域的构象表位,不具有病毒中和活​​性。与V3肽302-321结合的另外四个MAb表现出交叉反应性gp120结合和相对弱的病毒中和活​​性。这些单克隆抗体不仅在V3区域而且在V1 / V2环的底部都对氨基酸取代非常敏感,这意味着对表位的构象限制。最后一组9个单克隆抗体识别gp120 CD4结合位点附近的构象依赖性表位,并抑制gp120可溶性CD4相互作用。这九种单克隆抗体中的四种显示出对多种实验室适应的HIV-1菌株的广泛中和活性,其中三种仅中和了HIVIIIB,而两种亲和力较低的单克隆抗体未中和任何测试的菌株。总体而言,这项研究的结果表明,使用CD4-gp120复合物进行免疫可以引发针对构象敏感的gp120表位的抗体,其中一些抗体具有广泛的中和活性。我们建议用CD4-gp120复合物免疫可能值得进一步评估艾滋病疫苗的开发。

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