| CD3AK细胞过继免疫治疗的实验研究 |
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| 引用本文: | 孙瑛勋,程绍辉,于鸣,贺永怀,赖春宁,黎燕,沈倍奋.CD3AK细胞过继免疫治疗的实验研究[J].细胞与分子免疫学杂志,2005,21(2):218-221. |
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| 作者姓名: | 孙瑛勋 程绍辉 于鸣 贺永怀 赖春宁 黎燕 沈倍奋 |
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| 作者单位: | 军事医学科学院基础医学研究所,北京,100850 |
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| 摘 要: | 目的: 分析抗CD3分子的单克隆抗体 (mAb)yCD3的免疫学特性和生物学活性, 观察其激活的免疫活性细胞CD3AK体外及动物体内的抑瘤作用。方法: 用流式细胞术(FCM)测定yCD3的特异性, 以及CD3AK细胞的免疫表型和产生细胞因子的情况。用 3H -TdR法测定yCD3对淋巴细胞转化的作用; 乳酸脱氢酶法 (LDH)测定CD3AK细胞的体外细胞毒活性。建立荷瘤小鼠模型, 观察静脉注射CD3AK细胞后肿瘤生长的情况、转移灶数量和小鼠存活天数。结果: yCD3与T细胞呈特异性反应, 5μgyCD3可竞争抑制 70%的标准抗CD3抗体与细胞表面CD3分子的结合。yCD3刺激外周血淋巴细胞增殖的有效浓度为 8μg/L, 并与IL- 2、抗CD28抗体有协同作用。活化的CD3AK细胞中CD3 、CD8 和CD25 细胞增多; 产生IL- 2和IFN γ的CD3 细胞均有不同程度的增加, 在抗CD28抗体协同刺激下分别增加 3. 29和 2. 47倍。当效靶细胞比为 80∶1时, CD3AK细胞对体外肿瘤细胞杀伤的百分率为 57. 54%。分组观察荷瘤动物, CD3AK细胞治疗组的抑瘤率为 33. 17%, 对小鼠肿瘤肺转移的抑制率为39. 70%, 与LAK细胞联合治疗的疗效更显著。结论: yCD3可活化T细胞, 诱导的CD3AK细胞在体外及动物体内显示抑制肿瘤的作用, 在临床抗肿瘤过继性免疫治疗中具有重要意义。
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| 关 键 词: | 抗CD3单克隆抗体 CD3AK细胞 过继性免疫治疗 |
| 文章编号: | 1007-8738(2005)02-0218-04 |
| 修稿时间: | 2004年3月26日 |
Experimental study of adoptive immunotherapy using CD3AK cells |
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| SUN Ying-xun,CHENG Shao-hui,YU Ming,HE Yong-huai,LAI Chun-ning,LI Yan,SHEN Bei-fen.Experimental study of adoptive immunotherapy using CD3AK cells[J].Journal of Cellular and Molecular Immunology,2005,21(2):218-221. |
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| Authors: | SUN Ying-xun CHENG Shao-hui YU Ming HE Yong-huai LAI Chun-ning LI Yan SHEN Bei-fen |
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| Institution: | Institute of Basic Medicine, Academy of Military Medical Sciences, Beijing 100850, China. sunyx@amms.ac.cn |
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| Abstract: | AIM: To analyze the immunological properties and biological activity of a monoclonal antibody (mAb) against CD3 molecule(yCD3), and to observe the tumor-suppressive activity of CD3AK cells in vitro and in vivo. METHODS: FCM was used to test the specificity of yCD3 and the immunological phenotype and cytokine production of CD3AK. 3H-TdR assay was used to measure the transformation of lymphocytes activated by yCD3. LDH assay was used to analyze the cytotoxic activity of CD3AK in vitro. Mice bearing tumors were used to observe the anti-tumor effect of CD3AK cells. RESULTS: yCD3 could bind specifically to T cells. 5 microg yCD3 could competitively inhibit 70% of standard anti-CD3 antibody to bind with CD3 molecules on cell membrane. 8 microg/L of yCD3 stimulated the proliferation of peripheral blood lymphocytes, which could be further boosted by IL-2 or anti-CD28 antibodies. Among activated CD3AK cells, CD3+, CD8+, and CD25+ cells increased. IL-2 and IFN-gamma producing CD3+ cells were also increased, to 3.29- and 2.47- fold, respectively, under the co-stimulation of anti-CD28 antibody. When the ratio of effective cells and target cells was 80:1, 57.54% target cells were killed. As compared with control, the percent of tumor inhibition in CD3AK cells treated tumor-bearing mice was 33.17%, and the inhibition rate of lung metastasis was 39.70%. The CD3AK cells treatment was more effective when combined with LAK cells. CONCLUSION: yCD3 could activate T cells and significantly induce the tumor-suppressive activity of CD3AK cells in vitro and in vivo, which lays a foundation for adoptive immunotherapy against tumors in clinical medicine. |
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| Keywords: | anti-CD3 mAb CD3AK cell adoptive immunotherapy |
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