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首页> 外文期刊>Clinical and Translational Allergy >Expression profiling and functional analysis of Toll-like receptors in primary healthy human nasal epithelial cells shows no correlation and a refractory LPS response
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Expression profiling and functional analysis of Toll-like receptors in primary healthy human nasal epithelial cells shows no correlation and a refractory LPS response

机译:原发性健康人鼻上皮细胞中Toll样受体的表达谱和功能分析显示无相关性且难治性LPS反应

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摘要

Innate immune recognition via Toll-like receptors (TLRs) on barrier cells like epithelial cells has been shown to influence the regulation of local immune responses. Here we determine expression level variations and functionality of TLRs in nasal epithelial cells from healthy donors. Expression levels of the different TLRs on primary nasal epithelial cells from healthy donors derived from inferior turbinates was determined by RT-PCR. Functionality of the TLRs was determined by stimulation with the respective ligand and evaluation of released mediators by Luminex ELISA. Primary nasal epithelial cells express different levels of TLR1-6 and TLR9. We were unable to detect mRNA of TLR7, TLR8 and TLR10. Stimulation with Poly(I:C) resulted in a significant increased secretion of IL-4, IL-6, RANTES, IP-10, MIP-1β, VEGF, FGF, IL-1RA, IL-2R and G-CSF. Stimulation with PGN only resulted in significant increased production of IL-6, VEGF and IL-1RA. Although the expression of TLR4 and co-stimulatory molecules could be confirmed, primary nasal epithelial cells appeared to be unresponsive to stimulation with LPS. Furthermore, we observed huge individual differences in TLR agonist-induced mediator release, which did not correlate with the respective expression of TLRs. Our data suggest that nasal epithelium seems to have developed a delicate system of discrimination and recognition of microbial patterns. Hypo-responsiveness to LPS could provide a mechanism to dampen the inflammatory response in the nasal mucosa in order to avoid a chronic inflammatory response. Individual, differential expression of TLRs on epithelial cells and functionality in terms of released mediators might be a crucial factor in explaining why some people develop allergies to common inhaled antigens, and others do not.
机译:通过Toll样受体(TLR)对像上皮细胞这样的屏障细胞的先天免疫识别已显示会影响局部免疫反应的调节。在这里,我们确定来自健康供体的鼻上皮细胞中TLR的表达水平变化和功能。通过RT-PCR确定来自下鼻甲的健康供体的初级鼻上皮细胞上不同TLR的表达水平。通过用各自的配体刺激并通过Luminex ELISA评估释放的介质来确定TLR的功能。鼻上皮细胞表达不同水平的TLR1-6和TLR9。我们无法检测到TLR7,TLR8和TLR10的mRNA。用Poly(I:C)刺激导致IL-4,IL-6,RANTES,IP-10,MIP-1β,VEGF,FGF,IL-1RA,IL-2R和G-CSF的分泌显着增加。用PGN刺激只会导致IL-6,VEGF和IL-1RA的产生显着增加。尽管可以证实TLR4和共刺激分子的表达,但鼻腔上皮细胞似乎对LPS刺激无反应。此外,我们观察到了TLR激动剂诱导的介质释放的巨大个体差异,这与TLR的各自表达无关。我们的数据表明,鼻上皮似乎已经发展出一种区分和识别微生物模式的精密系统。对LPS的低反应性可以提供一种减轻鼻粘膜炎性反应的机制,以避免慢性炎性反应。上皮细胞上TLR的个体差异表达和释放介质的功能性可能是解释为什么某些人对常见吸入抗原产生过敏而其他人却没有的关键因素。

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