首页> 美国卫生研究院文献>Cancer Science >Granulocyte‐Macrophage Colony‐stimulating Factor Augments Lymphokine‐activated Killer Activity from Pleural Cavity Mononuclear Cells of Lung Cancer Patients without Malignant Effusion
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Granulocyte‐Macrophage Colony‐stimulating Factor Augments Lymphokine‐activated Killer Activity from Pleural Cavity Mononuclear Cells of Lung Cancer Patients without Malignant Effusion

机译:粒细胞巨噬细胞集落刺激因子增强肺癌患者胸腔单核细胞淋巴因子激活的杀伤活性无恶性积液

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摘要

The role of recombinant granulocyte‐macrophage colony‐stimulating factor (GM‐CSF) in augmentation of lymphokine‐activated killer (LAK) cell induction by interleukin‐2 (IL‐2) from pleural cavity mononuclear cells (PCMNCs) was examined in sixteen patients with resectable primary lung cancer not associated with malignant effusion. None of the patients had received any anticancer therapy prior to this study. Incubation of PCMNCs of patients without malignant effusion with GM‐CSF for 4 days in the presence of IL‐2 resulted in a significant increase in LAK activity against natural killer‐resistant Daudi cells. This result was obtained by using the 4 h 51Cr‐release assay. PCMNCs and blood mononuclear cells (BMNCs) were harvested simultaneously from pleural cavity lavage fluid and peripheral blood in lung cancer patients. The LAK activity developed from PCMNCs and BMNCs following incubation with IL‐2 for 4 days, but the LAK activity from PCMNCs was significantly lower than that from BMNCs (P < 0.05). Incubation of PCMNCs with GM‐CSF augmented the LAK activity from PCMNCs to a level as high as that from BMNCs. These results suggest that the combined use of GM‐CSF with IL‐2 may result in augmentation of LAK activity developed from PCMNCs of lung cancer patients without malignant effusion.
机译:在16例患者中检查了重组粒细胞巨噬细胞集落刺激因子(GM-CSF)在白细胞介素2(IL-2)从胸膜腔单核细胞(PCMNCs)诱导的淋巴因子激活的杀伤(LAK)细胞增强中的作用。可切除的原发性肺癌与恶性积液无关。在这项研究之前,没有患者接受过任何抗癌治疗。 IL-2存在下无恶性积液的GM-CSF患者的PCMNCs孵育4天导致ILK对天然杀伤性耐药Daudi细胞的活性显着增加。通过4 h 51 Cr释放分析获得了该结果。从肺癌患者的胸腔灌洗液和外周血中同时采集PCMNC和血液单核细胞(BMNC)。与IL-2孵育4天后,PCMNC和BMNC的LAK活性增强,但是PCMNC的LAK活性显着低于BMNC(P <0.05)。带有GM-CSF的PCMNC的孵化使PCMNC的LAK活动增加到与BMNC相同的水平。这些结果表明,GM-CSF与IL-2的联合使用可能导致肺癌患者无恶性积液的PCMNCs产生的LAK活性增强。

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