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High-throughput monitoring of human tumor-specific T-cell responses with large peptide pools

机译:高通量监测具有大型肽库的人类肿瘤特异性T细胞反应

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摘要

In immune intervention trials, the comprehensive investigation of immunogenicity or T-cell epitope-mapping is challenging especially when a large set of epitopes needs to be screened and limited sample material is available. To this end, T-cell responses are often monitored using peptide pools. Here, we assessed the magnitude and sensitivity of detection of antigen-specific CD8(+) and CD4(+) T cells using a single peptide alone or mixed into large pools. Interestingly the magnitude of ex vivo anti-viral and anti-tumor T-cell responses was identical irrespective of the presence and number of irrelevant peptides, in different functional assays with PBMCs from healthy donors and cancer patients. Moreover, the presence of up to 300 irrelevant peptides did not affect the threshold of responsiveness of antigen-specific CD8(+) T cells to single cognate peptides. These data demonstrate the relevance of using very large peptide pools for the sensitive and specific immune-monitoring of epitope-specific T cells in natural or immune-modulated context.
机译:在免疫干预试验中,对免疫原性或T细胞表位作图的全面研究具有挑战性,尤其是在需要筛选大量表位且样品材料有限的情况下。为此,经常使用肽库监测T细胞应答。在这里,我们评估了单独使用单个肽或混合成大肽对抗原特异性CD8(+)和CD4(+)T细胞的检测强度和敏感性。有趣的是,在健康捐献者和癌症患者的PBMC的不同功能测定中,不管无关肽的存在和数量如何,离体抗病毒和抗肿瘤T细胞反应的幅度都是相同的。此外,多达300个无关肽的存在不影响抗原特异性CD8(+)T细胞对单个同源肽的反应性阈值。这些数据证明了在自然或免疫调节的情况下,使用非常大的肽库对表位特异性T细胞的敏感和特异性免疫监测的相关性。

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