首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Characterization of functional and phenotypic changes in anti-Gag vaccine-induced T cell responses and their role in protection after HIV-1 infection
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Characterization of functional and phenotypic changes in anti-Gag vaccine-induced T cell responses and their role in protection after HIV-1 infection

机译:抗Gag疫苗诱导的T细胞反应的功能和表型变化的特征及其在HIV-1感染后的保护作用

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摘要

Worldwide HIV-1 vaccine efforts are guided by the principle that HIV-specific T cell responses may provide protection from infection or delay overt disease. However, no clear correlates of T cell-mediated immune protection have been identified. Here, we examine in a HLA-B27~+ HIV seronegative vaccinee persistent HIV-specific vaccine-induced anti-Gag CD4~+ and CD8~+ T cell responses. Although these responses exhibited those characteristics (multi-functionality, appropriate memory phenotype, and targeting of epitopes associated with long-term nonprogression) predicted to correlate with protection from infection, the subject became HIV infected. After HIV infection, the vaccine-induced CD8~+ T cells expanded, but both CD4~+ and CD8~+ T cell responses acquired the functional and phenotypic patterns characteristic of chronic HIV infection. The virus quickly escaped the vaccine-induced T cell response, and the subject progressed more rapidly than expected for someone expressing the HLA-B27 allele. These data suggest that control of HIV by vaccine-elicited HIV-specific T cell responses may be difficult, even when the T cell response has those characteristics predicted to provide optimal protection.
机译:全球HIV-1疫苗的努力遵循以下原则:HIV特异性T细胞反应可提供保护,防止感染或延缓明显疾病。然而,尚未鉴定出T细胞介导的免疫保护的明确关联。在这里,我们检查了HLA-B27〜+ HIV血清阴性疫苗中持续存在的HIV特异性疫苗诱导的抗Gag CD4〜+和CD8〜+ T细胞反应。尽管这些反应显示出与预防感染相关的特征(多功能,适当的记忆表型和靶向与长期无进展相关的表位),但该受试者已感染了HIV。 HIV感染后,疫苗诱导的CD8〜+ T细胞扩增,但CD4〜+和CD8〜+ T细胞反应均获得了慢性HIV感染的功能和表型特征。该病毒迅速逃脱了疫苗诱导的T细胞反应,并且该受试者的进展比表达HLA-B27等位基因的人的进展更快。这些数据表明,即使当T细胞反应具有预期可提供最佳保护的特征时,也很难通过疫苗引起的HIV特异性T细胞反应控制HIV。

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