首页> 外文OA文献 >Rapid changes in microRNA-146a expression negatively regulate the IL-1beta-induced inflammatory response in human lung alveolar epithelial cells.
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Rapid changes in microRNA-146a expression negatively regulate the IL-1beta-induced inflammatory response in human lung alveolar epithelial cells.

机译:microRNA-146a表达的快速变化对人肺泡上皮细胞中IL-1beta诱导的炎症反应产生负调控。

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摘要

Posttranscriptional regulation of gene expression by microRNAs (miRNAs) has been implicated in the regulation of chronic physiological and pathological responses. In this report, we demonstrate that changes in the expression of miRNAs can also regulate acute inflammatory responses in human lung alveolar epithelial cells. Thus, stimulation with IL-1beta results in a rapid time- and concentration-dependent increase in miRNA-146a and, to a lesser extent, miRNA-146b expression, although these increases were only observed at high IL-1beta concentration. Examination of miRNA function by overexpression and inhibition showed that increased miRNA-146a expression negatively regulated the release of the proinflammatory chemokines IL-8 and RANTES. Subsequent examination of the mechanism demonstrated that the action of miRNA-146a was mediated at the translational level and not through the down-regulation of proteins involved in the IL-1beta signaling pathway or chemokine transcription or secretion. Overall, these studies indicate that rapid increase in miRNA-146a expression provides a novel mechanism for the negative regulation of severe inflammation during the innate immune response.
机译:microRNA(miRNA)的基因表达的转录后调控已牵涉到慢性生理和病理反应的调控。在本报告中,我们证明了miRNA表达的变化也可以调节人肺泡上皮细胞的急性炎症反应。因此,用IL-1beta刺激导致miRNA-146a快速依赖时间和浓度的增加,而miRNA-146b表达则减少,尽管这些增加仅在高IL-1beta浓度下才能观察到。通过过度表达和抑制对miRNA功能的检查表明,增加的miRNA-146a表达会消极调节促炎性趋化因子IL-8和RANTES的释放。随后对该机制的检查表明,miRNA-146a的作用是在翻译水平上介导的,而不是通过下调参与IL-1beta信号通路或趋化因子转录或分泌的蛋白质来实现的。总体而言,这些研究表明,miRNA-146a表达的快速增加为先天免疫应答过程中严重炎症的负调控提供了新的机制。

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