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首页> 外文期刊>Retrovirology >Variations in autologous neutralization and CD4 dependence of b12 resistant HIV-1 clade C env clones obtained at different time points from antiretroviral na?ve Indian patients with recent infection
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Variations in autologous neutralization and CD4 dependence of b12 resistant HIV-1 clade C env clones obtained at different time points from antiretroviral na?ve Indian patients with recent infection

机译:在抗逆转录病毒Na've印度患者最近感染的不同时间点在不同时间点获得的自体中和和CD4依赖性的自体中和和CD4依赖性

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摘要

Background Limited information is available on HIV-1 Indian clade C sensitivities to autologous antibodies during the course of natural infection. In the present study, a total of 37 complete envelope clones (Env) were amplified at different time points predominantly from the plasma of five Indian patients with recent HIV-1 infection and envelope-pseudotyped viruses were examined for their magnitude of sensitivity to autologous plasma antibodies during natural course of infection. Results Variable low levels of neutralization were consistently detected with contemporaneous autologous plasma. In contrast to clade B and African clade C HIV-1 envelopes, Env clones obtained from four patients were found to be resistant to IgG1b12. The majority of the Env clones were resistant to 2G12 and 2F5 due to the absence of the minimal motifs required for antibody recognition, but were sensitive to 4E10. Nonetheless, Env clones from one patient were found to be sensitive to 2G12, atypical for clade C, and one Env clone exhibited unusual sensitivity to 17b, suggesting spontaneous exposure of CD4i epitopes. Phylogenetic analysis revealed that Env clones were closely clustered within patients. Variation in the potential N-linked glycosylation pattern also appeared to be different in patients over the course of infection. Interestingly, we found that the sensitivity of Envs to contemporaneous autologous NAbs correlated positively with increased sensitivity to soluble CD4 and inversely with anti-CD4 antibody and Envs with increased NAb sensitivity were able to efficiently infect HeLa cells expressing low CD4. Conclusion Our data showed considerable variations in autologous neutralization of these early HIV-1 clade C Envs in each of these patients and indicate greater exposure to CD4 of Envs that showed increased autologous neutralization. Interestingly, Env clones obtained from a single patient at different time points were found to retain sensitivity to b12 antibody that binds to CD4 binding site in Env in contrast to Envs obtained from other patients. However, we did not find any association between increased b12 sensitivity of Envs obtained from this particular patient with their degree of exposure to CD4.
机译:背景技术在自然感染过程中,在HIV-1印度支那型C敏感性上获得有限的信息。在本研究中,总共37种完全包络克隆(ENV)在不同的时间点,主要来自五种印度患者的血浆近期的HIV-1感染,并检查了对自体等离子体的敏感性程度的封装 - 假型病毒感染自然过程中的抗体。结果与当前自体等离子体一致检测变量低水平的中和。与CLADE B和非洲思潮CHIV-1信封形成鲜明对比,发现从四名患者获得的ENV克隆对IgG1B12抵抗力。由于抗体识别所需的最小基质,因此,大多数Env克隆耐药于2G12和2F5,但对4E10敏感。尽管如此,发现来自一个患者的ENV克隆对2G12敏感,对于胰蛋白C,非典型,并且一个ENV克隆对17B表现出不寻常的敏感性,表明CD4i表位的自发暴露。系统发育分析表明,Env克隆在患者内密切聚集。在感染过程中,潜在的N-连接的糖基化模式的变化也似乎不同。有趣的是,我们发现Envs对同期自体Nab的敏感性随着对可溶性CD4的敏感性和抗CD4抗体的敏感性而相关的敏感性,并且具有增加的Nab敏感性的envs能够有效地感染表达低CD4的Hela细胞。结论我们的数据表明,这些患者中每种早期的HIV-1 CRADE CEV中和的数据显示了相当大的变化,并表明更大的暴露于表现出增加自体中和的envs的CD4。有趣的是,发现从不同时间点的单个患者获得的ENV克隆对B12抗体保持敏感性,所述B12抗体与来自其他患者所获得的ENV的ENV4的CD4结合位点结合。然而,我们没有发现从该特定患者获得的B12 envs增加的敏感度之间的任何关联,其暴露于CD4。

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