首页> 外文期刊>International journal of biological sciences >MicroRNA-142-3p and let-7g Negatively Regulates Augmented IL-6 Production in Neonatal Polymorphonuclear Leukocytes
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MicroRNA-142-3p and let-7g Negatively Regulates Augmented IL-6 Production in Neonatal Polymorphonuclear Leukocytes

机译:MicroRNA-142-3p和let-7g负调控新生多形核白细胞中IL-6产生的增加。

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Neonatal PMN are qualitatively impaired in functions, yet they frequently reveal augmented inflammatory reactions during sepsis. Here, we hypothesized that PMN from newborns produce more IL-6 than those from adults under LPS stimulation, in which transcriptional or posttranscriptional regulation is involved in the altered expression. We found that neonatal PMN produced significantly higher IL-6 mRNA and protein than adult PMN. The higher IL-6 expression was not related to transcriptional but posttranscriptional regulation as the IL-6 expression was affected by the addition of cycloheximide but not actinomycin. To examine whether miRNA was involved in the IL-6 regulation of neonatal PMN, we surveyed differential displays of miRNAs that could potentially regulate IL-6 expression before and after LPS stimulation. Four miRNAs: hsa-miR-26a, hsa-miR-26b, hsa-miR-142-3p and hsa-let 7g decreased or increased after LPS treatment for 4 h. Further validation by qRT-PCR identified miR-26b, miR-142-3p and let-7g significantly changed in neonatal PMN after LPS stimulation. The functional verification by transfection of miR-142-3p and let-7g precursors into neonatal PMN significantly repressed the IL-6 mRNA and protein expression, suggesting that miR-142-3p and let-7g negatively regulate IL-6 expression in neonatal PMNs. Modulation of miRNA expression may be used to regulate IL-6 production in newborns with altered inflammatory reactions.
机译:新生儿PMN的功能在质量上受到损害,但它们经常显示败血症期间炎症反应加剧。在这里,我们假设在LPS刺激下,来自新生儿的PMN产生的IL-6比成年人产生的IL-6多,其中转录或转录后调控与表达的改变有关。我们发现,新生儿PMN产生的IL-6 mRNA和蛋白质明显高于成人PMN。较高的IL-6表达与转录无关,但转录后调控,因为IL-6表达受环己酰亚胺的影响,但不受放线菌素的影响。为了检查miRNA是否参与新生儿PMN的IL-6调节,我们调查了可能在LPS刺激之前和之后调节IL-6表达的miRNA的差异显示。 LPS处理4小时后,四种miRNA:hsa-miR-26a,hsa-miR-26b,hsa-miR-142-3p和hsa-let 7g减少或增加。通过qRT-PCR进一步验证,LPS刺激后,新生儿PMN中的miR-26b,miR-142-3p和let-7g发生了显着变化。通过将miR-142-3p和let-7g前体转染到新生儿PMN中进行的功能验证显着抑制了IL-6 mRNA和蛋白表达,表明miR-142-3p和let-7g对新生PMN中的IL-6表达负调控。 。 miRNA表达的调节可用于调节炎症反应改变的新生儿IL-6的产生。

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