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同种异体的细胞毒性T淋巴细胞诱导和培养
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作者 刘书钦 徐和德 《华南师范大学学报(自然科学版)》 CAS 1994年第4期1-11,共11页
通过诱导获得了移植的CTL(细胞毒性T淋巴细胞)并为建立大规模培养系统而研究了其培养条件,通过外周血单核细胞(PMBC)与经X-射线辐射的肿瘤SQ-5在含有白细胞介素(IL)1、2、4、6的Rhamα培养液中共同培养... 通过诱导获得了移植的CTL(细胞毒性T淋巴细胞)并为建立大规模培养系统而研究了其培养条件,通过外周血单核细胞(PMBC)与经X-射线辐射的肿瘤SQ-5在含有白细胞介素(IL)1、2、4、6的Rhamα培养液中共同培养3天以上,获得了抗人肺鳞状癌肿SQ-5的人的CTL.CTL杀伤靶细胞的靶效比是1.在含有人的血清白蛋白(HSA)培养液中这种CTL生长很快,保存3个月以后仍保持很高杀伤活性,达95%以上。与非靶的肿瘤细胞相比,CTL表现出对靶细胞的特异活性,在一个月内即可获得足够量的CTL(10 ̄(10)-10 ̄(11)个).这些结果表明应用培养的CTL治疗各种癌症是有良好前景的治疗技术。 展开更多
关键词 CTL 诱导 细胞毒性 T淋巴细胞 肿瘤细胞
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Fixed-Tumor Vaccine: A Practical Formulation with Cytokine-Microspheres for Protective and Therapeutic Antitumor Immunity
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作者 彭宝岗 梁力建 +5 位作者 刘书钦 黄洁夫 何强 吕明德 梁锦龙 大野忠夫 《The Chinese-German Journal of Clinical Oncology》 CAS 2003年第4期196-202,250,共8页
Objective: To study the protective and therapeutic antitumor immunity against hepatocellular carcinoma (HCC) with the fixed-tumor vaccine.Methods: A tumor vaccine consisting of fixed tumor cells or fixed tumor fragmen... Objective: To study the protective and therapeutic antitumor immunity against hepatocellular carcinoma (HCC) with the fixed-tumor vaccine.Methods: A tumor vaccine consisting of fixed tumor cells or fixed tumor fragments combined with sustained-releasers of cytokines and a non-toxic adjuvant was developed. C57BL/6J mice were immunized intra-dermally with the vaccine on day 0 and 7, followed by intrahepatic challenge with live Hepa 1–6 cells.Results: All of 15 nonimmunized control mice developed the hepatoma. Protection of mice immunized with fixed Hepa 1–6 cells and both of IL-2/GM-CSF microspheres or further mixed with TiterMax Gold reached 80% and 87%, respectively. Mass growth of the established tumors, vaccinated twice at 5 mm in diameter, the tumor of control animals continued to grow. However, 7–10 days after the second injection of the tumor vaccine, the tumor growth was suppressed in 9 of 10 mice and then markedly reduced. Complete tumor regression was observed in 60% (6/10) of mice. Splenocytes from the control mice were not able to lyse target Hepa 1–6 cells and other tumor cells. In contrast splenocytes from the vaccinated mice exhibited a 41% lytic activity against the Hepa 1–6 cells tested at an effector/target (E/T) ratio of 5, whereas they did not exhibited such activity against the melanoma cells (B16-F1), Lewis lung carcinoma cells (LLC), renal carcinoma cells (Renca), and bladder carcinoma cells (MBT-2). The cytotoxic activity was inhibited by the treatment with anti-CD3, anti-CD8, and anti-MHC-class I monoclonal antibodies but not with anti-CD4 and anti-MHC-class II antibodies. In the Phase-I clinical trial, vaccination of HCC patients with the autologous vaccine is a well-tolerated treatment and induces fixed tumor fragment-specific immunity.Conclusion: Fixed HCC vaccination elicited protective and therapeutic antitumor immunity against HCC. The tumor vaccine elicited antigen specific CTL response lysis of the target HCC was mediated by the typical MHC-class I restricted CD8+ T cells. Key words cancer vaccine - cytotoxic T lymphocyte - immunotherapy - hepatoma 展开更多
关键词 cancer vaccine cytotoxic T lymphocyte IMMUNOTHERAPY HEPATOMA
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