肺泡上皮细胞中芳基烃受体的激活可限制炎症并保护肺上皮细胞的完整性。

IF 3.6 3区 医学 Q2 IMMUNOLOGY
Elizabeth Zimmerman, Anne Sturrock, Christopher A Reilly, Katherine L Burrell-Gerbers, Kristi Warren, Mustafa Mir-Kasimov, Mingyang A Zhang, Megan S Pierce, My N Helms, Robert Paine
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引用次数: 0

摘要

芳基烃受体(AHR)是一种在肺部广泛表达的受体/转录因子。肺泡上皮表达的 AHR 的生理作用仍不清楚。在这项研究中,我们检验了肺泡上皮 AHR 活性在肺损伤和修复过程中调节炎症反应和维持肺泡完整性方面发挥重要作用的假设。AHR 在肺泡上皮细胞(AECs)中表达并具有活性。用内源性 AHR 配体 FICZ(5,11-二氢吲哚并[3,2-b] 咔唑-6-甲醛)激活 AHR 能显著抑制小鼠原代肺泡上皮细胞和 MLE-15 上皮细胞系在炎症刺激下的炎性细胞因子表达。在小鼠急性肺损伤的 LPS 模型中,FICZ 与 LPS 合用可抑制蛋白质渗漏,减少中性粒细胞在 BAL 液中的积聚,并抑制肺组织和 BAL 液中炎症细胞因子的表达。与炎症损伤后的愈合有关的是,AHR 的激活抑制了 TGF-β 诱导的上皮-间质转化相关基因的表达。用 shRNA 在原代 AECs 或 CRISPR-Cas-9 诱导的 MLE-15 细胞中敲除 AHR 会导致 α 平滑肌肌动蛋白(αSma)、Col1a1 和 Fn1 上调,并降低上皮基因 Col4a1 和 Sdc1 的表达。在划痕模型中,缺乏 AHR 的 MLE-15 克隆显示伤口闭合速度加快。用 FICZ 激活 AHR 可增强原代小鼠 AECs 的屏障功能(跨上皮电阻),并限制炎症损伤后跨上皮电阻的下降。通过调节炎症细胞因子的表达,AHR 在 AECs 中的激活可保护肺泡的完整性,同时增强屏障功能并限制应激诱导的间质基因的表达。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Aryl Hydrocarbon Receptor Activation in Pulmonary Alveolar Epithelial Cells Limits Inflammation and Preserves Lung Epithelial Cell Integrity.

The aryl hydrocarbon receptor (AHR) is a receptor/transcription factor widely expressed in the lung. The physiological roles of AHR expressed in the alveolar epithelium remain unclear. In this study, we tested the hypothesis that alveolar epithelial AHR activity plays an important role in modulating inflammatory responses and maintaining alveolar integrity during lung injury and repair. AHR is expressed in alveolar epithelial cells (AECs) and is active. AHR activation with the endogenous AHR ligand, FICZ (5,11-dihydroindolo[3,2-b] carbazole-6-carboxaldehyde), significantly suppressed inflammatory cytokine expression in response to inflammatory stimuli in primary murine AECs and in the MLE-15 epithelial cell line. In an LPS model of acute lung injury in mice, coadministration of FICZ with LPS suppressed protein leak, reduced neutrophil accumulation in BAL fluid, and suppressed inflammatory cytokine expression in lung tissue and BAL fluid. Relevant to healing following inflammatory injury, AHR activation suppressed TGF-β-induced expression of genes associated with epithelial-mesenchymal transition. Knockdown of AHR in primary AECs with shRNA or in CRISPR-Cas-9-induced MLE-15 cells resulted in upregulation of α-smooth muscle actin (αSma), Col1a1, and Fn1 and reduced expression of epithelial genes Col4a1 and Sdc1. MLE-15 clones lacking AHR demonstrated accelerated wound closure in a scratch model. AHR activation with FICZ enhanced barrier function (transepithelial electrical resistance) in primary murine AECs and limited decline of transepithelial electrical resistance following inflammatory injury. AHR activation in AECs preserves alveolar integrity by modulating inflammatory cytokine expression while enhancing barrier function and limiting stress-induced expression of mesenchymal genes.

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来源期刊
Journal of immunology
Journal of immunology 医学-免疫学
CiteScore
8.20
自引率
2.30%
发文量
495
审稿时长
1 months
期刊介绍: The JI publishes novel, peer-reviewed findings in all areas of experimental immunology, including innate and adaptive immunity, inflammation, host defense, clinical immunology, autoimmunity and more. Special sections include Cutting Edge articles, Brief Reviews and Pillars of Immunology. The JI is published by The American Association of Immunologists (AAI)
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