J C Voltarelli, A A Rayner, M R Garovoy, D P Stites
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引用次数: 0
摘要
用重组白细胞介素-2 (IL-2)刺激正常人外周血或脾脏单核细胞,监测其表型标记和细胞毒性功能;1500 U /毫升)。新鲜脾细胞中自然杀伤细胞(CD3-NKH1+)含量低于5%,经IL-2活化后增加约3倍。在脾脏和外周血培养中,具有NKH1标记的T细胞在所有细胞类型中显示出最高的相对增量。来自外周血和脾脏的淋巴因子激活杀伤细胞(LAK)对K562、Daudi和COLO癌细胞表现出非常相似的细胞毒活性。三个目标在培养的7天内被杀死。在培养2 ~ 14 d时,循环和脾LAK细胞介导了抗体依赖性细胞对b细胞系的细胞毒性。细胞分选实验表明,K562靶点可被CD5+NKH1+和CD5-NKH1+细胞杀死,而Daudi靶点仅被脾脏和外周血中CD5-NKH1+活化的NK细胞杀死。综上所述,人脾脏LAK细胞具有与循环LAK细胞相似的表型和功能特性,它们可能用于人类癌症的过继免疫治疗。
Human spleen and peripheral blood lymphocytes activated by interleukin-2 have similar phenotypic and functional characteristics.
Phenotypic markers and cytotoxic function were monitored in cultures of normal human mononuclear cells obtained from peripheral blood or spleen and stimulated by recombinant interleukin-2 (IL-2; 1,500 U/ml). Fresh spleen cells contained less than 5% natural killer (NK) cells (CD3-NKH1+), which increased about threefold after activation with IL-2. In both spleen and peripheral blood cultures, T cells with the NKH1 marker showed the highest relative increment among all cell types studied. Lymphokine-activated killer (LAK) cells from peripheral blood and spleen displayed very similar cytotoxic activity against K562, Daudi, and COLO carcinoma cell lines. Killing of the three targets peaked at 7 days of culture. Antibody-dependent cell cytotoxicity against a B-cell line was mediated by both circulating and splenic LAK cells from 2 to 14 days of culture. Cell sorting experiments showed that K562 targets were killed by both CD5+NKH1+ and CD5-NKH1+ cells whereas Daudi targets are only killed by CD5-NKH1+ activated NK cells from both spleen and peripheral blood. In summary, human spleen LAK cells have similar phenotypic and functional properties to circulating LAK cells, and they may be used for adoptive immunotherapy of human cancer.