Lactoferrin interacts with SPLUNC1 to attenuate lipopolysaccharide-induced inflammation of human nasal epithelial cells via down-regulated MEK1/2-MAPK signaling.

Yung‐An Tsou, Y. Tung, Tsu-Fang Wu, G. Chang, Han-Chien Chen, Chia-Der Lin, Chih-Ho Lai, Hsiao‐Ling Chen, Chuan‐Mu Chen
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引用次数: 14

Abstract

The short palate, lung, and nasal epithelium clone 1 (SPLUNC1) protein is an important innate material in the upper airway, and lactoferrin (LF) aids the innate functions in humans. In this study, a nasal epithelial model was used to investigate how LF modulates SPLUNC1 to reduce the inflammatory process mediated by lipopolysaccharide (LPS). The inflammation of human RPMI-2650 cells was induced with LPS to evaluate SPLUNC1 expression after treating the cells with bovine LF (bLF). The interaction pathway between LF and SPLUNC1 in LPS-induced inflammation was further investigated. Our study reveals that the addition of bLF results in the recovery of SPLUNC1 expression in nasal epithelial cells under LPS-induced inflammation. MAPK is involved in the main pathway for the SPLUNC1 and bLF interaction. Decreased SPLUNC1 function could be recovered by addition of bLF. The MEK1/2-MAPK signaling pathway is crucial for the SPLUNC1 and bLF interaction. Therefore, LF could support SPLUNC1 in the innate immunity recovery process.
乳铁蛋白与SPLUNC1相互作用,通过下调MEK1/2-MAPK信号通路,减弱脂多糖诱导的人鼻上皮细胞炎症。
短腭、肺和鼻上皮克隆1 (SPLUNC1)蛋白是上呼吸道重要的先天物质,而乳铁蛋白(LF)有助于人类的先天功能。本研究采用鼻上皮模型研究LF如何调节SPLUNC1以减少脂多糖(LPS)介导的炎症过程。用牛LF (bLF)处理人rpm -2650细胞后,用LPS诱导细胞炎症,评价SPLUNC1的表达。进一步研究LF与SPLUNC1在lps诱导炎症中的相互作用途径。我们的研究表明,在lps诱导的炎症下,添加bLF可使鼻上皮细胞中SPLUNC1的表达恢复。MAPK参与SPLUNC1和bLF相互作用的主要途径。添加bLF可恢复SPLUNC1功能下降。MEK1/2-MAPK信号通路对于SPLUNC1和bLF相互作用至关重要。因此,LF可以在先天免疫恢复过程中支持SPLUNC1。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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