B7-1 (cd80)共刺激诱导自体肿瘤特异性细胞毒性t淋巴细胞对人肾癌细胞系的活性

Journal of immunotherapy with emphasis on tumor immunology : official journal of the Society for Biological Therapy Pub Date : 1996-01-01 DOI:10.1097/00002371-199601000-00001

Y C Wang, L Zhu, R McHugh, S D Graham, C D Hillyer, D Dillehay, K W Sell, P Selvaraj

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引用次数: 36

摘要

最近的小鼠模型显示，肿瘤细胞上共刺激分子如B7-1的表达可以诱导肿瘤特异性免疫，这表明修饰表达共刺激分子的肿瘤细胞可能是一种潜在的肿瘤疫苗。为了探讨B7-1共刺激在诱导人类自体肿瘤免疫中的重要性，我们建立了一个来自肿瘤切除的肾癌细胞系RCC-1，并在体外研究了患者的抗肿瘤免疫反应。RCC-1细胞系组成性表达主要组织相容性复合体(MHC) I类、细胞间粘附分子(ICAM)-1和白细胞功能相关抗原(LFA)-3分子，MHC II类分子在体外通过干扰素γ (ifn - γ)处理诱导。然而，RCC-1和ifn - γ处理的RCC-1细胞均未表达B7-1，并且在混合淋巴细胞和肿瘤细胞反应(MLTR)实验中均未能诱导t细胞增殖反应，这表明细胞粘附分子如ICAM-1和LFA-3提供的共刺激信号不足以引发抗肿瘤免疫反应。然而，在MLTR实验中，将人B7-1转染到RCC-1中，这些细胞能够诱导显著的t细胞增殖。这种t细胞反应可以通过抗b7单抗治疗肿瘤细胞而被阻断。在体外，RCC- 1b7细胞也诱导亲本RCC-1细胞产生肿瘤特异性的细胞溶解T淋巴细胞，而不相关的RCC系A498或自体植物血凝素(PHA)母细胞几乎没有非特异性的细胞溶解。这种特异性细胞毒性可通过抗cd8单抗和补体治疗消除。总之，我们的研究表明，B7-1-CD28相互作用在诱导人类自体肿瘤特异性细胞毒性T淋巴细胞(CTL)中起着关键作用，这表明共刺激分子转染的肿瘤细胞可能有助于在体外扩增肿瘤特异性自体CTL，用于过继性肿瘤免疫治疗。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Induction of autologous tumor-specific cytotoxic T-lymphocyte activity against a human renal carcinoma cell line by B7-1 (CD8O) costimulation.

Recently mouse models have shown that expression of costimulatory molecules such as B7-1 on tumor cells can induce tumor-specific immunity, suggesting that tumor cells modified to express costimulatory molecules can be a potential tumor vaccine. To investigate the importance of B7-1 co-stimulation in induction of autologous tumor immunity in humans, we established a renal carcinoma cell line, RCC-1, from a tumor resection and studied the patient's antitumor immune responses in vitro. The RCC-1 cell line constitutively expressed major histocompatibility complex (MHC) class I, intercellular adhesion molecule (ICAM)-1, and leukocyte function-associated antigen (LFA)-3 molecules, and MHC class II molecules were induced by interferon-gamma (IFN-gamma) treatment in vitro. However, neither RCC-1- nor IFN-gamma-treated RCC-1 cells expressed B7-1, and both failed to induce T-cell proliferative responses in mixed lymphocyte and tumor cell reaction (MLTR) assays, suggesting that the costimulatory signals provided by cell adhesion molecules such as ICAM-1 and LFA-3 were not sufficient to elicit an antitumor immune response. However, on transfection of the human B7-1 into RCC-1, these cells were able to induce a significant T-cell proliferation in MLTR assays. This T-cell response could be blocked by anti-B7 mAb treatment of the tumor cells. RCC-1B7 cells also induced the generation of tumor-specific cytolytic T lymphocytes to the parent RCC-1 cells in vitro, with little nonspecific cytolysis of an unrelated RCC line, A498, or autologous phytohemagglutinin (PHA) blasts. This specific cytotoxicity could be abrogated by anti-CD8 mAb and complement treatment. In summary, our study indicates that B7-1-CD28 interaction plays a critical role in induction of autologous tumor-specific cytotoxic T lymphocytes (CTLs) in humans, suggesting that the costimulatory molecule transfected tumor cells could be useful in expanding tumor-specific autologous CTL in vitro for adoptive tumor immunotherapy.

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Journal of immunotherapy with emphasis on tumor immunology : official journal of the Society for Biological Therapy

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