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Isolation and characterization of a novel neutralizing antibody targeting the CD4-binding site of HIV-1 gp120

机译:靶向HIV-1 gp120 CD4结合位点的新型中和抗体的分离与鉴定

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Isolation and characterization of novel HIV-1 neutralizing antibodies assists the development of effective AIDS vaccines and immune therapeutics. In this study, we constructed a phage display antibody library by using the PBMC samples of a Glade B' HIV-1-infected long-term nonprogressor (LTNP) whose sera exhibited broadly neutralizing activity. A novel human monoclonal antibody (hMAb), termed A16, was identified by panning the library with two clades of HIV-1 Env glycoproteins. We demonstrated that A16 neutralized 32% of 73 tested HIV-1 isolates and it targeted the CD4-binding site (CD4bs) of gp120 with high affinity. By selecting the peptide mimotopes in combination with computational algorithms and site-directed mutagenesis, the epitope of A16 was mapped to the structurally conserved sites located within the beta 1-alpha 1, loop D, beta 20-beta 21 (bridging sheet) and beta 24-alpha 5 of gp120, which critically determine the CD4 binding and are involved in the epitopes of CD4bs-directed antibodies. Our studies have shed new insights for the immune response of HIV-1 infection and offered a new tool for designing vaccine immunogens and antibody-based immune therapy. (C) 2016 Elsevier B.V. All rights reserved.
机译:新型HIV-1中和抗体的分离和鉴定有助于开发有效的AIDS疫苗和免疫疗法。在这项研究中,我们通过使用Glade B'HIV-1感染的长期非进展者(LTNP)的PBMC样品构建了噬菌体展示抗体文库,该血清的血清具有广泛的中和活性。通过用两个进化枝HIV-1 Env糖蛋白淘选文库,鉴定了一种新型人类单克隆抗体(hMAb),称为A16。我们证明了A16中和了73个测试过的HIV-1分离株中的32%,并以高亲和力靶向gp120的CD4结合位点(CD4bs)。通过与计算算法和定点诱变结合选择肽模拟表位,将A16的表位定位到位于beta 1-alpha 1,loop D,beta 20-beta 21(桥接片)和beta中的结构保守位点gp120的24-alpha 5,它决定性地确定CD4的结合并参与CD4bs定向抗体的表位。我们的研究为HIV-1感染的免疫反应提供了新见解,并为设计疫苗免疫原和基于抗体的免疫疗法提供了新工具。 (C)2016 Elsevier B.V.保留所有权利。

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