il -2活化淋巴细胞对恶性疾病的过继免疫治疗。

Biken journal Pub Date : 1987-06-01

Y Kimoto, T Taguchi

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引用次数: 0

摘要

利用重组白细胞介素2 (TGP-3)诱导淋巴因子活化的杀伤细胞(LAK细胞)或白细胞介素2 (IL-2)活化的杀伤细胞用于临床恶性疾病的过继免疫治疗。外周血淋巴细胞(PBL)与IL-2和正常人血浆孵育1-2周后获得LAK细胞，该细胞对靶细胞表现出最大的细胞毒性，并且不需要毒性剂量的IL-2来增强或维持其细胞毒性。自体和异体LAK细胞均用于5例临床病例，无任何免疫副作用，3例有效。

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Adoptive immunotherapy of malignant diseases with IL-2-activated lymphocytes.

Lymphokine activated killer cells (LAK cells) or interleukin 2 (IL-2)-activated killer cells were induced by recombinant IL-2 (TGP-3) for clinical adoptive immunotherapy of malignant diseases. After incubation of peripheral blood lymphocytes (PBL) with IL-2 and normal human plasma for 1-2 weeks LAK cells were obtained that showed a maximum cytotoxicity against target cells, and did not need a toxic dose of IL-2 to enhance or maintain their cytotoxicity. Both autologous and allogeneic LAK cells were used in five clinical cases without any immune side effects, and were effective in three cases.

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Biken journal

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