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Identification and characterization of HIV-1-specific CD8+ T cell epitopes presented by HLA-A*2601

机译:HLA-A * 2601呈现的HIV-1特异性CD8 + T细胞表位的鉴定和表征

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Since HLA-A*26 is one of the most common alleles in Asia, where approximately 20% of people have this allele, identification of HIV-1-specific epitopes presented by HLA-A*26 is necessary for studies on the immunopathogenesis of AIDS and vaccine development in Asia. As presented herein, we used the reverse immunogenetics approach to identify HIV-1 epitopes presented by HLA-A*2601, one of the major HLA-A*26 subtypes. We selected 24 HLA-A*2601-binding peptides out of 110 HIV-1 peptides by using a HLA-A*2601 stabilization assay. The ability of these HLA-A*2601-binding peptides to induce peptide-specific CD8(+) T cells was tested by stimulating PBMCs from HIV-1-infected individuals having HLA-A*2601 with these peptides. Four HLA-A*2601-binding peptides induced peptide-specific CD8 T cells. Analysis using HIV-1 recombinant vaccinia-infected C1R-A*2601 cells indicated that these four peptides were HIV-1 epitopes endogenously presented by HLA-A*2601. Two epitope-specific CD8(+) T cells were predominantly detected in HIV-1 infected individuals, suggesting that these epitopes may be useful for vaccine development.
机译:由于HLA-A * 26是亚洲最常见的等位基因之一,大约有20%的人患有该等位基因,因此对HLA-A * 26呈现的HIV-1特异性表位进行鉴定对于研究AIDS的免疫发病机理是必要的和亚洲的疫苗开发。如本文所述,我们使用了反向免疫遗传学方法来鉴定由HLA-A * 2601(一种主要的HLA-A * 26亚型)呈现的HIV-1表位。通过使用HLA-A * 2601稳定化分析,我们从110个HIV-1肽中选择了24个HLA-A * 2601结合肽。这些HLA-A * 2601结合肽诱导肽特异性CD8(+)T细胞的能力通过用这些肽刺激HIV-1感染的具有HLA-A * 2601的个体的PBMC来测试。四个HLA-A * 2601结合肽诱导了肽特异性CD8 T细胞。使用HIV-1重组牛痘感染的C1R-A * 2601细胞进行的分析表明,这四个肽是HLA-A * 2601内源性呈递的HIV-1表位。在HIV-1感染的个体中主要检测到两个抗原决定簇特异性CD8(+)T细胞,表明这些抗原决定簇可能对疫苗开发有用。

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