Irsicaixa AIDS Research Institute-HIVACAT, Badalona, Spain.
J Transl Med. 2011 Dec 7;9:208. doi: 10.1186/1479-5876-9-208.
The efficacy of the CTL component of a future HIV-1 vaccine will depend on the induction of responses with the most potent antiviral activity and broad HLA class I restriction. However, current HIV vaccine designs are largely based on viral sequence alignments only, not incorporating experimental data on T cell function and specificity.
Here, 950 untreated HIV-1 clade B or -C infected individuals were tested for responses to sets of 410 overlapping peptides (OLP) spanning the entire HIV-1 proteome. For each OLP, a "protective ratio" (PR) was calculated as the ratio of median viral loads (VL) between OLP non-responders and responders.
For both clades, there was a negative relationship between the PR and the entropy of the OLP sequence. There was also a significant additive effect of multiple responses to beneficial OLP. Responses to beneficial OLP were of significantly higher functional avidity than responses to non-beneficial OLP. They also had superior in-vitro antiviral activities and, importantly, were at least as predictive of individuals' viral loads than their HLA class I genotypes.
The data thus identify immunogen sequence candidates for HIV and provide an approach for T cell immunogen design applicable to other viral infections.
未来 HIV-1 疫苗的 CTL 成分的疗效将取决于诱导具有最强抗病毒活性和广泛 HLA Ⅰ类限制的反应。然而,目前的 HIV 疫苗设计在很大程度上仅基于病毒序列比对,而不结合 T 细胞功能和特异性的实验数据。
在这里,950 名未经治疗的 HIV-1 型 B 或 C 感染者接受了针对整个 HIV-1 蛋白组的 410 个重叠肽(OLP)集的反应测试。对于每个 OLP,计算“保护比”(PR)作为 OLP 无反应者和反应者之间中位病毒载量(VL)的比值。
对于两个 clade,PR 与 OLP 序列的熵之间存在负相关。对有益的 OLP 的多个反应也存在显著的加性效应。有益的 OLP 的反应比非有益的 OLP 的反应具有更高的功能亲和力。它们还具有更好的体外抗病毒活性,重要的是,与 HLA Ⅰ类基因型相比,它们至少能更好地预测个体的病毒载量。
因此,这些数据确定了 HIV 的免疫原序列候选物,并提供了一种适用于其他病毒感染的 T 细胞免疫原设计方法。
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