人重组单核细胞趋化与活化因子及脂多糖对人血液单核细胞抗肿瘤活性的协同作用。

Lymphokine and cytokine research Pub Date : 1993-10-01
R K Singh, I J Fidler
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引用次数: 0

摘要

单核细胞趋化和激活因子(MCAF)是单核细胞募集到慢性炎症和肿瘤部位的重要介质。在本研究中,我们确定了MCAF是否也能增强单核细胞的杀肿瘤能力。与MCAF和亚阈值浓度的脂多糖(LPS)孵养的人单核细胞对同种异体A375黑色素瘤细胞表现出协同杀瘤活性,无论其转移潜力如何。MCAF和LPS处理的顺序至关重要。先用MCAF处理4小时,然后用LPS处理18小时的单核细胞对黑色素瘤细胞具有高度的细胞毒性,而先用LPS处理然后再用MCAF处理的单核细胞则没有。用MCAF和LPS处理单核细胞也显著增加了肿瘤坏死因子的产生。这些数据表明,与干扰素- γ一样,MCAF可以诱导人类单核细胞对LPS产生反应。白细胞介素-8,一种中性粒细胞的趋化因子,并没有增强单核细胞的lps触发的肿瘤杀伤反应。总的来说,这些数据表明MCAF可以影响血液单核细胞的募集和肿瘤杀伤激活。因此,MCAF可能是肿瘤消退的重要介质。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Synergism between human recombinant monocyte chemotactic and activating factor and lipopolysaccharide for activation of antitumor properties in human blood monocytes.

Monocyte chemotactic and activating factor (MCAF) is an important mediator of monocyte recruitment to sites of chronic inflammation and neoplasia. In the present study, we determined whether MCAF can also enhance the activation of tumoricidal capacity of monocytes. Human monocytes incubated with MCAF and subthreshold concentrations of lipopolysaccharide (LPS) exhibited synergistic tumoricidal activity against allogeneic A375 melanoma cells, irrespective of their metastatic potential. The sequence of MCAF and LPS treatment was crucial. Monocytes treated first with MCAF for 4 h and then with LPS for 18 h were highly cytotoxic to the melanoma cells, whereas monocytes first treated with LPS and then with MCAF were not. Treatment of monocytes with MCAF and LPS also significantly increased production of tumor necrosis factor. These data suggest that like interferon-gamma, MCAF can prime human monocytes to respond to LPS. Interleukin-8, a chemokine for neutrophils, did not enhance the monocytes' LPS-triggered tumoricidal response. Collectively, these data show that MCAF can influence the recruitment and tumoricidal activation of blood monocytes. Therefore, MCAF may be an important mediator of tumor regression.

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