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中和印度 HIV-1 感染者的 Tier-2 病毒和鉴定血浆抗体的表位图谱。

Neutralization of tier-2 viruses and epitope profiling of plasma antibodies from human immunodeficiency virus type 1 infected donors from India.

机构信息

Department of Biochemistry, C N Centre, All India Institute of Medical Sciences, New Delhi, India.

出版信息

PLoS One. 2012;7(8):e43704. doi: 10.1371/journal.pone.0043704. Epub 2012 Aug 31.

DOI:10.1371/journal.pone.0043704
PMID:22952740
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3432049/
Abstract

Broadly cross neutralizing antibodies (NAbs) are generated in a group of HIV-1 infected individuals during the natural infection, but little is known about their prevalence in patients infected with viral subtypes from different geographical regions. We tested here the neutralizing efficiency of plasma antibodies from 80 HIV-1 infected antiretroviral drug naive patients against a panel of subtype-B and C tier 2 viruses. We detected cross-neutralizing antibodies in approximately 19-27% of the plasma, however the subtype-C specific neutralization efficiency predominated (p = 0.004). The neutralizing activity was shown to be exclusively mediated by the immunoglobulin G (IgG) fraction in the representative plasma samples. Epitope mapping of three, the most cross-neutralizing plasma (CNP) AIIMS206, AIIMS239 and AIIMS249 with consensus-C overlapping envelope peptides revealed ten different binding specificities with only V3 and IDR being common. The V3 and IDR were highly antigenic regions but no correlation between their reciprocal Max50 binding titers and neutralization was observed. In addition, the neutralizing activity of CNP was not substantially reduced by V3 and gp41 peptides except a modest contribution of MPER peptide. The MPER was rarely recognized by plasma antibodies though antibody depletion and competition experiments demonstrated MPER dependent neutralization in two out of three CNP. Interestingly, the binding specificity of one of the CNP (AIIMS206) overlapped with broadly neutralizing mAb 2F5 epitope. Overall, the data suggest that, despite the low immunogenicity of HIV-1 MPER, the antibodies directed to this region may serve as crucial reagents for HIV-1 vaccine design.

摘要

广谱中和抗体(NAbs)在一组 HIV-1 感染个体的自然感染中产生,但对于来自不同地理区域的病毒亚型感染患者中其流行率知之甚少。我们在此测试了 80 名未经抗逆转录病毒药物治疗的 HIV-1 感染患者的血浆抗体对一组 B 型和 C 型 2 级病毒的中和效率。我们在大约 19-27%的血浆中检测到了交叉中和抗体,但 C 型特异性中和效率占主导地位(p = 0.004)。在代表性的血浆样本中,中和活性被证明仅由免疫球蛋白 G(IgG)部分介导。用共识-C 重叠包膜肽对三种最具交叉中和活性的血浆(CNP)AIIMS206、AIIMS239 和 AIIMS249 进行表位作图,揭示了十种不同的结合特异性,只有 V3 和 IDR 是共同的。V3 和 IDR 是高度抗原性区域,但它们的相互 Max50 结合滴度和中和之间没有相关性。此外,CNP 的中和活性不会因 V3 和 gp41 肽而明显降低,除了 MPER 肽的适度贡献外。MPER 很少被血浆抗体识别,尽管抗体耗竭和竞争实验表明,在三种 CNP 中有两种依赖于 MPER 的中和。有趣的是,其中一种 CNP(AIIMS206)的结合特异性与广泛中和单克隆抗体 2F5 的表位重叠。总体而言,数据表明,尽管 HIV-1 MPER 的免疫原性较低,但针对该区域的抗体可能是 HIV-1 疫苗设计的关键试剂。

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