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Promiscuous Recognition of a Trypanosoma cruzi CD8 + T Cell Epitope among HLA-A2, HLA-A24 and HLA-A1 Supertypes in Chagasic Patients

机译:甲壳类患者HLA-A2,HLA-A24和HLA-A1超型之间的克氏锥虫CD8 + T细胞表位的混杂识别

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摘要

Background\ud\udTcTLE is a nonamer peptide from Trypanosoma cruzi KMP-11 protein that is conserved among different parasite strains and that is presented by different HLA-A molecules from the A2 supertype. Because peptides presented by several major histocompatibility complex (MHC) supertypes are potential targets for immunotherapy, the aim of this study was to determine whether MHC molecules other than the A2 supertype present the TcTLE peptide.\udMethodology/Principal Findings\ud\udFrom 36 HLA-A2-negative chagasic patients, the HLA-A genotypes of twenty-eight patients with CD8+ T cells that recognized the TcTLE peptide using tetramer (twenty) or functional (eight) assays, were determined. SSP-PCR was used to identify the A locus and the allelic variants. Flow cytometry was used to analyze the frequency of TcTLE-specific CD8+ T cells, and their functional activity (IFN-γ, TNFα, IL-2, perforin, granzyme and CD107a/b production) was induced by exposure to the TcTLE peptide. All patients tested had TcTLE-specific CD8+ T cells with frequencies ranging from 0.07–0.37%. Interestingly, seven of the twenty-eight patients had HLA-A homozygous alleles: A*24 (5 patients), A*23 (1 patient) and A*01 (1 patient), which belong to the A24 and A1 supertypes. In the remaining 21 patients with HLA-A heterozygous alleles, the most prominent alleles were A24 and A68. The most common allele sub-type was A*2402 (sixteen patients), which belongs to the A24 supertype, followed by A*6802 (six patients) from the A2 supertype. Additionally, the A*3002/A*3201 alleles from the A1 supertype were detected in one patient. All patients presented CD8+ T cells producing at least one cytokine after TcTLE peptide stimulation.\udConclusion/Significance\ud\udThese results show that TcTLE is a promiscuous peptide that is presented by the A24 and A1 supertypes, in addition to the A2 supertype, suggesting its potential as a target for immunotherapy.
机译:背景\ ud \ udTcTLE是克氏锥虫KMP-11蛋白的九聚体肽,在不同的寄生虫菌株中均保守,并由来自A2超型的不同HLA-A分子呈现。由于几种主要的组织相容性复合体(MHC)超型呈现的肽是免疫治疗的潜在靶标,因此本研究的目的是确定除A2超型以外的MHC分子是否存在TcTLE肽。\ udMethodology / Principal Findings \ ud \ ud来自36 HLA -A2阴性无门诊患者,确定了28位CD4 + T细胞的HLA-A基因型,这些患者使用四聚体(二十种)或功能性(八种)检测方法识别了TcTLE肽。 SSP-PCR用于鉴定A基因座和等位基因变体。流式细胞仪用于分析TcTLE特异性CD8 + T细胞的频率,并通过暴露于TcTLE肽诱导其功能活性(IFN-γ,TNFα,IL-2,穿孔素,颗粒酶和CD107a / b产生)。所有接受测试的患者均具有TcTLE特异性CD8 + T细胞,频率范围为0.07–0.37%。有趣的是,在28位患者中,有7位具有HLA-A纯合等位基因:A * 24(5位患者),A * 23(1位患者)和A * 01(1位患者),分别属于A24和A1超型。在其余的21位HLA-A杂合等位基因患者中,最突出的等位基因是A24和A68。最常见的等位基因亚型是A * 2402(十六名患者),属于A24超型,其次是A * 6802(六名患者),来自A2超型。此外,在一名患者中检测到来自A1超型的A * 3002 / A * 3201等位基因。所有患者均表现出CD8 + T细胞在TcTLE肽刺激后产生至少一种细胞因子。\ ud结论/意义\ ud \ ud这些结果表明,除了A2超型外,TcTLE是由A24和A1超型呈递的混杂肽。其作为免疫疗法靶标的潜力。

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