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γ干扰素对体外分化的人巨噬细胞白细胞介素-1分泌的影响。

The effect of gamma interferon on IL-1 secretion of in vitro differentiated human macrophages.

作者信息

Haq A U, Rinehart J J, Maca R D

出版信息

J Leukoc Biol. 1985 Dec;38(6):735-46. doi: 10.1002/jlb.38.6.735.

DOI:10.1002/jlb.38.6.735
PMID:3934302
Abstract

After being cultured overnight, human monocytes lose their ability to secrete interleukin-1 (IL-1) when stimulated by lipopolysaccharide (LPS). However, when these monocytes were cultured for up to 9 days with various concentrations of interferon-gamma (IFN-gamma), these cells were found to retain their ability to secrete appreciable amounts of IL-1 on LPS stimulation. However, the effect was observed only if the monocytes were exposed to the IFN before LPS stimulation and simultaneous addition of IFN and LPS to macrophages was ineffective. This effect of IFN-gamma was related to the concentration of IFN added to the cultures and was completely neutralized by a monoclonal antibody to IFN-gamma. In addition to inducing IL-1 secretion, IFN-gamma also appeared to increase the overall production of IL-1, since reinduction of IL-1 secretion was not associated with a decrease in intracellular IL-1 content. When these macrophages were initially cultured with IFN-gamma, washed, and further cultured with IFN free medium, these macrophages were found to progressively lose their capacity to secrete IL-1 in response to LPS. Conversely, when monocytes were initially cultured in medium free of IFN, washed, and then further cultured in new medium, but now containing IFN-gamma, these macrophages were found to regain their capacity to secrete IL-1. However, the amount of reinduced IL-1 secretion decreased as the length of the initial culture period without IFN increased, with less than optimal IL-1 secretion occurring if monocytes were allowed to mature for 6 days before IFN-gamma pretreatment. In summary, these studies suggest that IFN-gamma may be important in enhancing IL-1 production and secretion by maturing macrophages and tissue macrophages and consequently may play a role in regulating the accessory cell activity of these cells for a variety of immune responses in vivo.

摘要

人单核细胞经一夜培养后,在受到脂多糖(LPS)刺激时会丧失分泌白细胞介素-1(IL-1)的能力。然而,当这些单核细胞在含有不同浓度干扰素-γ(IFN-γ)的条件下培养长达9天时,发现这些细胞在LPS刺激下仍保留分泌相当数量IL-1的能力。但是,只有在单核细胞在LPS刺激之前暴露于IFN时才会观察到这种效应,同时向巨噬细胞中添加IFN和LPS则无效。IFN-γ的这种效应与添加到培养物中的IFN浓度有关,并且可被抗IFN-γ单克隆抗体完全中和。除了诱导IL-1分泌外,IFN-γ似乎还增加了IL-1的总体产生,因为IL-1分泌的再次诱导与细胞内IL-1含量的减少无关。当这些巨噬细胞最初用IFN-γ培养、洗涤后,再用不含IFN的培养基进一步培养时,发现这些巨噬细胞逐渐丧失了对LPS刺激分泌IL-1的能力。相反,当单核细胞最初在不含IFN的培养基中培养、洗涤后,然后在含有IFN-γ的新培养基中进一步培养时,发现这些巨噬细胞恢复了分泌IL-1的能力。然而,随着初始无IFN培养期的延长,再次诱导的IL-1分泌量会减少,如果单核细胞在IFN-γ预处理前成熟6天,则IL-1分泌量低于最佳水平。总之,这些研究表明,IFN-γ可能在增强成熟巨噬细胞和组织巨噬细胞的IL-1产生和分泌方面很重要,因此可能在体内调节这些细胞对多种免疫反应的辅助细胞活性中发挥作用。

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