Kumar Sanjeev, Kumar Rajesh, Khan Lubina, Makhdoomi Muzamil Ashraf, Thiruvengadam Ramachandran, Mohata Madhav, Agarwal Mudit, Lodha Rakesh, Kabra Sushil Kumar, Sinha Subrata, Luthra Kalpana
Department of Biochemistry, All India Institute of Medical Sciences, New Delhi, India.
Department of Pediatrics, All India Institute of Medical Sciences, New Delhi, India.
Front Immunol. 2017 Nov 15;8:1568. doi: 10.3389/fimmu.2017.01568. eCollection 2017.
Progression of human immunodeficiency virus type-1 (HIV-1) infection in children is faster than adults. HIV-1 subtype C is responsible for more than 50% of the infections globally and more than 90% infections in India. To date, there is no effective vaccine against HIV-1. Recent animal studies and human Phase I trials showed promising results of the protective effect of anti-HIV-1 broadly neutralizing antibodies (bnAbs). Interaction between CD4 binding site (CD4bs) on the HIV-1 envelope glycoprotein and CD4 receptor on the host immune cells is the primary event leading to HIV-1 infection. The CD4bs is a highly conserved region, comprised of a conformational epitope, and is a potential target of bnAbs such as VRC01 that is presently under human clinical trials. Recombinant scFvs can access masked epitopes due to their small size and have shown the potential to inhibit viral replication and neutralize a broad range of viruses. Pediatric viruses are resistant to many of the existing bnAbs isolated from adults. Therefore, in this study, pooled peripheral blood mononuclear cells from 9 chronically HIV-1 subtype C infected pediatric cross-neutralizers whose plasma antibodies exhibited potent and cross-neutralizing activity were used to construct a human anti-HIV-1 scFv phage library of 9 × 10 individual clones. Plasma mapping using CD4bs-specific probes identified the presence of CD4bs directed antibodies in 4 of these children. By extensive biopanning of the library with CD4bs-specific antigen RSC3 core protein, we identified two cross-neutralizing scFv monoclonals 2B10 and 2E4 demonstrating a neutralizing breadth and GMT of 77%, 17.9 µg/ml and 32%, 51.2 µg/ml, respectively, against a panel of 49 tier 1, 2 and 3 viruses. Both scFvs competed with anti-CD4bs bnAb VRC01 confirming their CD4bs epitope specificity. The 2B10 scFv was effective in neutralizing the 7 subtype C and subtype A pediatric viruses tested. Somatic hypermutations in the VH gene of scFvs (10.1-11.1%) is comparable with that of the adult antibodies. These cross-neutralizing CD4bs-directed scFvs can serve as potential reagents for passive immunotherapy. A combination of cross-neutralizing scFvs of diverse specificities with antiretroviral drugs may be effective in suppressing viremia at an early stage of HIV-1 infection and prevent disease progression.
儿童人类免疫缺陷病毒1型(HIV-1)感染的进展比成人更快。HIV-1 C亚型在全球超过50%的感染病例中起作用,在印度超过90%的感染病例中起作用。迄今为止,尚无针对HIV-1的有效疫苗。最近的动物研究和人类I期试验显示了抗HIV-1广泛中和抗体(bnAbs)具有保护作用的有前景的结果。HIV-1包膜糖蛋白上的CD4结合位点(CD4bs)与宿主免疫细胞上的CD4受体之间的相互作用是导致HIV-1感染的主要事件。CD4bs是一个高度保守的区域,由一个构象表位组成,是bnAbs(如目前正在进行人体临床试验的VRC01)的潜在靶点。重组单链抗体片段(scFvs)因其尺寸小能够接触到隐蔽表位,并已显示出抑制病毒复制和中和多种病毒的潜力。儿科病毒对许多从成人中分离出的现有bnAbs具有抗性。因此,在本研究中,来自9名慢性HIV-1 C亚型感染儿科交叉中和者的外周血单个核细胞被汇集,这些患儿的血浆抗体表现出强效和交叉中和活性,用于构建一个包含9×10个个体克隆的人抗HIV-1 scFv噬菌体文库。使用CD4bs特异性探针进行血浆图谱分析确定了其中4名儿童中存在针对CD4bs的抗体。通过用CD4bs特异性抗原RSC3核心蛋白对文库进行广泛的生物淘选,我们鉴定出两种交叉中和scFv单克隆抗体2B10和2E4,它们对一组49种1、2和3级病毒的中和广度和几何平均滴度(GMT)分别为77%、17.9μg/ml和32%、51.2μg/ml。两种scFvs都与抗CD4bs bnAb VRC01竞争,证实了它们的CD4bs表位特异性。2B10 scFv在中和所测试的7种C亚型和A亚型儿科病毒方面有效。scFvs的重链可变区(VH)基因中的体细胞超突变(10.1 - 11.1%)与成人抗体相当。这些针对CD4bs的交叉中和scFvs可作为被动免疫治疗的潜在试剂。具有不同特异性的交叉中和scFvs与抗逆转录病毒药物联合使用可能在HIV-1感染早期有效抑制病毒血症并预防疾病进展。
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