In vitro influence of endotoxin on human mononuclear phagocyte structure and function. 2. Enhancement of the expression of cytoststic and cytolytic activity of normal and lymphokine-activated monocytes.

J Hammerstrøm
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Abstract

The presence of non-toxic concentrations of E. coli endotoxin (LPS) during the in vitro interaction of normal human monocytes and a human tumour cell line (NHIK 3025) enhanced monocyte-mediated target cell cytostasis and cytolysis. Monocyte responsiveness to LPS was greatest at an intermediate stage of in vitro differentiation. The expression of cytostatic and cytolytic activity by human monocytes activated with mediators from Corynebacterium parvum-stimulated human lymphocytes was also enhanced by LPS. Lymphokine activation did not induce additional LPS responsiveness in the monocytes. Monocytes activated with lymphokines and subsequently deactivated by in vitro culture did not show any increase in LPS responsiveness. A soluble cytostatic factor, which is probably not cold thymidine, was released from monocytes exposed first to lymphokines and then to LPS. While LPS is ineffective as an induction signal of monocyte cytotoxicity to tumour cells in this system, it enhances the expression of cytotoxicity induced by prolonged in vitro culture or lymphokine activation.

内毒素对人单核吞噬细胞结构和功能的体外影响。2. 增强正常和淋巴因子活化单核细胞的细胞增殖和细胞溶解活性的表达。
在正常人类单核细胞和人类肿瘤细胞系(NHIK 3025)的体外相互作用中,无毒浓度的大肠杆菌内毒素(LPS)的存在增强了单核细胞介导的靶细胞的细胞停滞和细胞溶解。单核细胞对LPS的反应在体外分化的中间阶段是最大的。由细小棒状杆菌刺激的人淋巴细胞的介质激活的人单核细胞的细胞抑制和细胞溶解活性的表达也被LPS增强。淋巴因子激活不会诱导单核细胞产生额外的LPS反应。单核细胞被淋巴因子激活,随后被体外培养失活,没有显示出LPS反应性的任何增加。一种可溶性的细胞抑制因子,可能不是冷胸腺嘧啶,首先暴露于淋巴因子,然后暴露于LPS的单核细胞释放。在该系统中,LPS作为单核细胞对肿瘤细胞毒性的诱导信号是无效的,但它可以增强体外培养时间延长或淋巴因子激活诱导的细胞毒性的表达。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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