首页> 外文期刊>European Journal of Immunology >Frequent occurrence of high affinity T cells against MELOE-1 makes this antigen an attractive target for melanoma immunotherapy.
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Frequent occurrence of high affinity T cells against MELOE-1 makes this antigen an attractive target for melanoma immunotherapy.

机译:频繁发生的高亲和力的T细胞针对MELOE-1使这种抗原具有吸引力黑色素瘤免疫治疗的目标。

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摘要

We recently showed that the infusion of tumor infiltrating lymphocytes specific for the MELOE-1 antigen was associated with a prolonged relapse-free survival for HLA-A2(+) melanoma patients who received tumor infiltrating lymphocytes therapy. Here, we characterized the MELOE-1/A2-specific T-cell repertoire in healthy donors and melanoma patients to further support an immunotherapy targeting this epitope. Using tetramer enrichment followed by multicolor staining, we found that MELOE-1-specific T cells were present in the blood of healthy donors and patients at similar frequencies (around 1 in 1x10(5) CD8(+) cells). These cells mainly displayed a naive phenotype in 4/6 healthy donors and 3/6 patients, whereas high proportions of memory cells were observed in the remaining individuals of both groups. There was a recurrent usage of the Valpha12.1 chain for 17/18 MELOE-1-specific T-cell clones derived from healthy donors or patients, associated with diverse Vbeta chains and V(D)J junctional sequences. All clones derived from melanoma patients (9/9) were reactive against the MELOE-1(36-44) peptide and against HLA-A2(+) melanoma cell lines. This study documents the existence of a large TCR repertoire specific for the MELOE-1/A2 epitope and its capacity to give rise to antitumor CTL that supports the development of immunotherapies targeting this epitope.
机译:我们最近显示,肿瘤的灌注浸润淋巴细胞MELOE-1所特有的抗原与长期黑色素瘤复发存活率为hla a2 (+)病人肿瘤的浸润淋巴细胞疗法。MELOE-1 / A2-specific t细胞在健康的曲目捐助者和黑色素瘤患者进一步的支持一个免疫疗法针对这种抗原决定基。四聚物浓缩多色紧随其后染色,我们发现MELOE-1-specific T细胞在场的血液健康的捐赠者和吗患者相似的频率(约11 x10 (5) CD8(+)细胞)。显示一个天真的表型在4/6健康的捐赠者和3/6的病人,而高的比例在剩下的记忆细胞观察个人的团体。使用Valpha12.1链的17/18MELOE-1-specific t细胞克隆来自健康的捐赠者或病人,联系在一起不同Vβ链和V (D) J交界序列。(9/9)的患者反应对MELOE-1(36-44)肽和hla a2 (+)黑素瘤细胞系。大细胞剧目特定的存在MELOE-1 / A2抗原决定基及其提供的能力抗肿瘤细胞毒性t淋巴细胞,支持免疫疗法的发展目标表位。

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