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内源性白细胞介素-1对人单核细胞中I-309基因表达的调控

Regulation of I-309 gene expression in human monocytes by endogenous interleukin-1.

作者信息

Selvan R S, Zhou L J, Krangel M S

机构信息

Department of Immunology, Duke University Medical Center, Durham, NC 27710, USA.

出版信息

Eur J Immunol. 1997 Mar;27(3):687-94. doi: 10.1002/eji.1830270317.

DOI:10.1002/eji.1830270317
PMID:9079810
Abstract

Activated human monocytes are a source of numerous beta-chemokines. The present study was conducted to determine whether these cells produce the human beta-chemokine I-309 and to compare the induction requirements of I-309 to those of other beta-chemokines. We demonstrate that appropriately stimulated adherence-purified human peripheral blood monocytes express I-309 transcripts and secreted I-309 protein. Two stimuli, immobilized IgG and lipopolysaccharide (LPS), synergize strongly to induce I-309 gene expression. We further demonstrate that the production of endogenous interleukin (IL)-1alpha plays a crucial role in I-309 induction. Thus, neutralization of endogenous IL-1alpha using an anti-IL-1alpha antiserum inhibits the induction of I-309 transcripts in response to stimulation with immobilized IgG and LPS, and exogenous IL-1alpha or IL-1beta induces I-309 transcripts in monocytes stimulated with immobilized IgG. Immobilized IgG and LPS have the opposite effect on monocyte chemoattractant protein-1 (MCP-1) gene expression, in that the induction observed with either stimulus alone is diminished using the two stimuli in combination. Furthermore, endogenous and exogenous IL-1 can be either stimulatory or inhibitory for MCP-1 gene expression depending on other signals delivered to the monocytes. Immobilized IgG and LPS synergize to induce macrophage inflammatory protein-1alpha transcripts, but endogenous IL-1 does not play a significant role. Thus, each of these beta-chemokine genes is under distinct regulatory control in human monocytes.

摘要

活化的人单核细胞是多种β趋化因子的来源。本研究旨在确定这些细胞是否产生人β趋化因子I-309,并比较I-309与其他β趋化因子的诱导需求。我们证明,经适当刺激的贴壁纯化人外周血单核细胞表达I-309转录本并分泌I-309蛋白。两种刺激物,固定化IgG和脂多糖(LPS),强烈协同诱导I-309基因表达。我们进一步证明内源性白细胞介素(IL)-1α的产生在I-309诱导中起关键作用。因此,使用抗IL-1α抗血清中和内源性IL-1α可抑制固定化IgG和LPS刺激后I-309转录本的诱导,而外源性IL-1α或IL-1β可在固定化IgG刺激的单核细胞中诱导I-309转录本。固定化IgG和LPS对单核细胞趋化蛋白-1(MCP-1)基因表达有相反的作用,即单独使用任何一种刺激物观察到的诱导在两种刺激物联合使用时会减弱。此外,内源性和外源性IL-1对MCP-1基因表达的作用可能是刺激或抑制,这取决于传递给单核细胞的其他信号。固定化IgG和LPS协同诱导巨噬细胞炎性蛋白-1α转录本,但内源性IL-1不起重要作用。因此,这些β趋化因子基因中的每一个在人单核细胞中都受到不同的调控。

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