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Differential expression of cytokine transcripts in neonatal and adult ovine alveolar macrophages in response to respiratory syncytial virus or toll-like receptor ligation

机译:新生儿呼吸道合胞病毒或通行费样受体结扎反应在新生和成年绵羊肺泡巨噬细胞中细胞因子转录子的差异表达

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摘要

Alveolar macrophages (AMϕs) secrete regulatory molecules that are believed to be critical in maintaining normal lung homeostasis. However, in response to activating signals, AMϕs have been shown to become highly phagocytic cells capable of secreting significant levels of pro-inflammatory cytokines. There is evidence to suggest that susceptibility of Mϕ subpopulations to viral infection, and their subsequent cytokine/chemokine response, is dependent on age of the host. In the present study, we compared bovine respiratory syncytial virus (BRSV) replication and induction of cytokine responses in neonatal ovine AMϕs to those cells isolated from adult animals. While neonatal AMϕs could be infected with BRSV, viral replication was limited as previously shown for AMϕs from mature animals. Interestingly, following BRSV infection, peak mRNA levels of IL-1β and IL-8 in neonatal AMϕ were several fold higher than levels induced in adult AMϕs. In addition, peak mRNA expression for the cytokines examined occurred at earlier time points in neonatal AMϕs compared to adult AMϕs. However, the data indicated that viral replication was not required for the induction of specific cytokines in either neonatal or adult AMϕs. TLR3 and TLR4 agonists induced significantly higher levels of cytokine transcripts than BRSV in both neonatal and adult AMϕs. It was recently proposed that immaturity of the neonatal immune system extends from production of pro-inflammatory cytokines to regulation of such responses. Differential regulation of cytokines in neonatal AMϕs compared to adult AMϕs in response to RSV could be a contributory factor to more severe clinical episodes seen in neonates.
机译:肺泡巨噬细胞(AMϕ)分泌调节分子,据信对于维持正常的肺动态平衡至关重要。然而,响应激活信号,AMϕ已被证明是能够吞噬大量促炎细胞因子的高度吞噬细胞。有证据表明,M +亚群对病毒感染的敏感性及其随后的细胞因子/趋化因子反应取决于宿主的年龄。在本研究中,我们比较了牛呼吸道合胞病毒(BRSV)的复制和新生绵羊AMϕ中细胞因子反应的诱导与从成年动物分离的那些细胞的比较。尽管新生儿AMϕs可能被BRSV感染,但病毒复制受到限制,如先前对成熟动物的AMϕs所示。有趣的是,在BRSV感染后,新生AMϕ中IL-1β和IL-8的峰值mRNA水平比成年AMϕs诱导的水平高几倍。此外,与成人AMϕs相比,新生儿AMϕs中检测到的细胞因子的峰值mRNA表达出现在更早的时间点。但是,数据表明在新生儿或成人AMϕs中诱导特定细胞因子不需要病毒复制。在新生儿和成人AMϕs中,TLR3和TLR4激动剂诱导的细胞因子转录物水平均显着高于BRSV。最近有人提出,新生儿免疫系统的不成熟从促炎性细胞因子的产生扩展到这种反应的调节。与成人AMϕs对RSV的反应相比,新生儿AMϕs中细胞因子的差异调节可能是导致新生儿中出现更严重临床发作的一个因素。

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