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首页> 外文期刊>Vaccine >Memory CD8(+) T cells elicited by HIV-1 lipopeptide vaccines display similar phenotypic profiles but differences in term of magnitude and multifunctionality compared with FLU- or EBV-specific memory T cells in humans
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Memory CD8(+) T cells elicited by HIV-1 lipopeptide vaccines display similar phenotypic profiles but differences in term of magnitude and multifunctionality compared with FLU- or EBV-specific memory T cells in humans

机译:HIV-1脂肽疫苗引发的记忆CD8(+)T细胞表现出相似的表型特征,但与人类中FLU或EBV特异性记忆T细胞相比,其大小和多功能性方面存在差异

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Differentiation marker, multifunctionality and magnitude analyses of specific-CD8(+) memory T cells are crucial to improve development of HIV vaccines designed to generate cell-mediated immunity. Therefore, we fully characterized the HIV-specific CD8(+) T cell responses induced in volunteers vaccinated with HIV lipopeptide vaccines for phenotypic markers, tetramer staining, cytokine secretion, and cytotoxic activities. The frequency of ex vivo CD8+ T cells elicited by lipopeptide vaccines is very rare and central-memory phenotype and functions of these cells were been shown to be important in AIDS immunity. So, we expanded them using specific peptides to compare the memory T cell responses induced in volunteers by HIV vaccines with responses to influenza (FLU) or Epstein Barr virus (EBV). By analyzing the differentiation state of IFN-gamma-secreting CD8(+) T cells, we found a CCR7(-)CD45RA(-)CD28(+int)/CD28(-) profile (>85%) belonging to a subset of intermediate-differentiated effector T cells for HIV, FLU, and EBV. We then assessed the quality of the response by measuring various T cell functions. The percentage of single IFN-gamma T cell producers in response to HIV was 62% of the total of secreting T cells compared with 35% for FLU and EBV, dual and triple (IFN-gamma/IL-2/CD107a) T cell producers could also be detected but at lower levels (8% compared with 37%). Finally, HIV-specific T cells secreted IFN-gamma and TNF-alpha, but not the dual combination like FLU- and EBV-specific T cells. Thus, we found that the functional profile and magnitude of expanded HIV-specific CD8(+) T precursors were more limited than those of to FLU- and EBV-specific CD8(+) T cells. These data show that CD8(+) T cells induced by these HIV vaccines have a similar differentiation profile to FLU and EBV CD8(+) T cells, but that the vaccine potency to induce multifunctional T cells needs to be increased in order to improve vaccination strategies
机译:特异性CD8(+)记忆T细胞的分化标记,多功能性和强度分析对于改善旨在产生细胞介导的免疫力的HIV疫苗的开发至关重要。因此,我们充分表征了在用HIV脂肽疫苗接种疫苗的志愿者中诱导的HIV特异性CD8(+)T细胞应答的表型标记,四聚体染色,细胞因子分泌和细胞毒活性。脂肽疫苗引起的离体CD8 + T细胞的频率非常罕见,并且这些细胞的中枢记忆表型和功能已显示对AIDS免疫非常重要。因此,我们使用特定的肽扩展了它们,以比较艾滋病毒疫苗在志愿者中诱导的记忆T细胞反应与对流感(FLU)或爱泼斯坦巴尔病毒(EBV)的反应。通过分析分泌IFN-γ的CD8(+)T细胞的分化状态,我们发现CCR7(-)CD45RA(-)CD28(+ int)/ CD28(-)谱(> 85%)属于以下子集HIV,FLU和EBV的中间分化效应T细胞。然后,我们通过测量各种T细胞功能来评估反应的质量。单一的IFN-γT细胞产生者对HIV的反应占总分泌T细胞的62%,而FLU和EBV,双重和三重(IFN-γ/ IL-2 / CD107a)T细胞产生者所占的百分比为35%也可以检测到,但含量较低(8%比37%)。最后,HIV特异性T细胞分泌IFN-γ和TNF-α,但不像FLU和EBV特异性T细胞那样双重结合。因此,我们发现扩展的HIV特异性CD8(+)T前体的功能谱和大小比FLU-和EBV特异性CD8(+)T细胞的局限性更大。这些数据表明,由这些HIV疫苗诱导的CD8(+)T细胞与FLU和EBV CD8(+)T细胞具有相似的分化特征,但是需要提高疫苗诱导多功能T细胞的能力以改善疫苗接种情况策略

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