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首页> 外文期刊>British Journal of Cancer >Generation of adherent lymphokine activated killer (A-LAK) cells from patients with acute myelogenous leukaemia
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Generation of adherent lymphokine activated killer (A-LAK) cells from patients with acute myelogenous leukaemia

机译:从急性骨髓性白血病患者中产生粘附性淋巴因子激活的杀伤细胞(A-LAK)

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Successful generation of adherent lymphokine-activated killer (A-LAK) cells, highly-enriched in CD3-CD56+ antitumour effector cells, from the peripheral blood of ten patients with acute myelogenous leukaemia (AML) is described. The AML patients were either untreated or in remission. In vitro proliferation of A-LAK cells in patients with AML was generally poor, unless the cells were cocultured with irradiated concanavalin A (ConA)--prestimulated allogeneic PBL or selected lymphoblastoid cell lines (LCL) as feeder cells. Using this method, the median fold proliferation was 290 for A-LAK cells cultured with ConA-activated feeders and 291 for those grown with LCL, both significantly higher (both P less than 0.001) than the median of 2-fold expansion observed in cultures without feeders. A-LAK cultures generated in the presence of feeders consistently showed good enrichment (up to 90%) in CD3-CD56+ NK cells. Although NK activity was not significantly increased on a per cell basis in A-LAK cells grown with feeder cells, total lytic activities against both NK-sensitive target, K562, and NK-resistant target, Daudi, were significantly greater (P less than 0.02 for ConA-PBL feeders and P less than 0.005 for LCL feeders) as compared to those in paired cultures without feeders. In the presence of irradiated allogeneic feeder cells, 7/10 AML patients generated A-LAK cultures characterised by good proliferation and increased purity as well as cytotoxic activity.
机译:描述了成功地从十位急性骨髓性白血病(AML)患者的外周血中成功产生了高度富含CD3-CD56 +抗肿瘤效应细胞的粘附淋巴因子激活的杀伤(A-LAK)细胞。 AML患者未经治疗或已缓解。 AML患者中A-LAK细胞的体外增殖通常较差,除非将细胞与辐照伴刀豆球蛋白A(ConA)预先刺激的同种异体PBL或选定的成淋巴细胞样细胞系(LCL)共培养作为饲养细胞。使用这种方法,用ConA激活的饲养细胞培养的A-LAK细胞的中位增殖为290,而用LCL生长的细胞为291,两者均显着高于(均小于0.001)培养中观察到的2倍增长的中值。没有支线。在饲养细胞存在下产生的A-LAK培养物在CD3-CD56 + NK细胞中始终表现出良好的富集(高达90%)。尽管在与饲养细胞一起生长的A-LAK细胞中NK活性在每个细胞上均未显着增加,但针对NK敏感靶标K562和NK抗性靶标Daudi的总裂解活性明显更高(P小于0.02对于ConA-PBL饲养者,PCL饲养者的P小于0.005)。在辐照的同种异体饲养细胞的存在下,7/10 AML患者产生了特征在于良好增殖和增加的纯度以及细胞毒性活性的A-LAK培养物。

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