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首页> 外文期刊>The journal of immunology >Up-Regulation of CCR2 Chemokine Receptor Expression and Increased Susceptibility to the Multitropic HIV Strain 89.6 in Monocytes Exposed to Glucocorticoid Hormones
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Up-Regulation of CCR2 Chemokine Receptor Expression and Increased Susceptibility to the Multitropic HIV Strain 89.6 in Monocytes Exposed to Glucocorticoid Hormones

机译:糖皮质激素激素暴露的单核细胞中CCR2趋化因子受体表达的上调和对多态HIV株89.6的敏感性增加

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Glucocorticoid hormones (GC) are potent antiinflammatory agents widely used in the treatment of diverse human diseases. The present study was aimed at assessing the effect of GC on chemokine receptor expression in human monocytes. Dexamethasone (Dex) up-regulated mRNA expression of the monocyte chemotactic protein (MCP-1, CCL2) chemokine receptor CCR2. The effect was selective in that other chemokine receptors were not substantially affected. Stimulation by Dex was observed after 4 h of exposure at concentrations of 10?7 to 10?5 M. Steroids devoid of GC activity were inactive, and the GC receptor antagonist, RU486, inhibited stimulation. Dex did not affect the rate of nuclear transcription, but augmented the CCR2 mRNA half-life. Augmentation of CCR2 expression by Dex was associated with increased chemotaxis. Finally, Dex treatment induced productive replication of the HIV strain 89.6, which utilizes CCR2 as entry coreceptor, in freshly isolated monocytes. Together with previous findings, these results indicate that at least certain pro- and antiinflammatory molecules have reciprocal and divergent effects on expression of a major monocyte chemoattractant, MCP-1, and of its receptor (CCR2). Augmentation of monocyte CCR2 expression may underlie unexplained in vivo effects of GC as well as some of their actions on HIV infection.
机译:糖皮质激素(GC)是有效的抗炎药,广泛用于治疗多种人类疾病。本研究旨在评估GC对人单核细胞趋化因子受体表达的影响。地塞米松(Dex)上调了单核细胞趋化蛋白(MCP-1,CCL2)趋化因子受体CCR2的mRNA表达。该作用是选择性的,因为其他趋化因子受体基本上没有受到影响。暴露4小时后,在10?7至10?5 M的浓度下,观察到Dex的刺激。没有GC活性的类固醇失活,GC受体拮抗剂RU486抑制了刺激。 Dex不会影响核转录的速率,但会延长CCR2 mRNA的半衰期。 Dex增强CCR2表达与趋化性增加有关。最终,Dex处理诱导了HIV菌株89.6在新鲜分离的单核细胞中的有效复制,该菌株利用CCR2作为进入共受体。与以前的发现一起,这些结果表明,至少某些促炎和抗炎分子对主要单核细胞趋化剂MCP-1及其受体(CCR2)的表达具有相互和不同的作用。单核细胞CCR2表达的增强可能是GC无法解释的体内效应及其对HIV感染的某些作用的基础。

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