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首页> 外文期刊>Clinical immunology: The official journal of the Clinical Immunology Society >MHC-I-restricted melanoma antigen specific TCR-engineered human CD4+ T cells exhibit multifunctional effector and helper responses, in vitro.
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MHC-I-restricted melanoma antigen specific TCR-engineered human CD4+ T cells exhibit multifunctional effector and helper responses, in vitro.

机译:MHC-I限制的黑色素瘤抗原特异性TCR工程化的人CD4 + T细胞在体外表现出多功能效应和辅助反应。

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摘要

MHC class I-restricted human melanoma epitope MART-1(27-35) specific TCR-engineered CD4+CD25- T cells synthesize Th1 type cytokines and exhibit cytolytic effector function upon cognate stimulation. A detailed characterization of such TCR-engineered CD4+CD25- T cells now reveals that they are multifunctional. For example, they undergo multiple rounds of division, synthesize cytokines (IFN-gamma, TNF-alpha, IL-2, and MIP1ss), lyse target cells, and "help" the expansion of the MART-1(27-35) specific CD8+ T cells when stimulated by the MART-1(27-35) peptide pulsed DC. Multiparametric analyses reveal that a single TCR-engineered CD4+ T cell can perform as many as five different functions. Nearly 100% MART-1(27-35) specific TCR expressing CD4+ T cells can be generated through retroviral vector-based transduction and one round of in vitro stimulation by the peptide pulsed DC. MHC class I-restricted tumor epitope specific TCR transduced CD4+ T cells, therefore, could be useful in immunotherapeutic strategies for melanoma or other human malignancies.
机译:MHC I类限制的人类黑素瘤抗原决定簇MART-1(27-35)特异性TCR工程改造的CD4 + CD25-T细胞合成Th1型细胞因子,并在同源刺激下表现出溶细胞效应功能。现在,对此类TCR工程改造的CD4 + CD25-T细胞的详细表征表明它们具有多功能性。例如,它们经历多轮分裂,合成细胞因子(IFN-γ,TNF-alpha,IL-2和MIP1ss),裂解靶细胞并“帮助” MART-1(27-35)特异性扩增当受MART-1(27-35)肽脉冲DC刺激时,CD8 + T细胞。多参数分析表明,单个TCR工程改造的CD4 + T细胞可以执行多达五种不同的功能。可以通过基于逆转录病毒载体的转导和肽脉冲DC进行的一轮体外刺激来产生近100%表达MART-1(27-35)的TCR特异性CD4 + T细胞。因此,MHC I类限制的肿瘤抗原决定簇特异性TCR转导的CD4 + T细胞可用于黑色素瘤或其他人类恶性肿瘤的免疫治疗策略。

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