短链脂肪酸通过眼部 G 蛋白偶联受体 43 抑制角膜对 TLR 配体的炎症反应

IF 5.9 1区 医学 Q1 OPHTHALMOLOGY
Jun Wu , Nu Chen , Elizabeth Grau , Luke Johnson , Yongqing Liu , Chi Li , Patrick A. Scott , Chang Kim , Deming Sun , Henry J. Kaplan , Hui Shao
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引用次数: 0

摘要

目的众所周知,肠道微生物群产生的短链脂肪酸(SCFAs)可通过G-蛋白偶联受体(GPR)43部分调节免疫,从而在肠道平衡中发挥主要作用。我们利用 TLR 配体诱导的小鼠角膜炎模型,研究了 SCFAs 和 GPR43 是否在眼部炎症反应的发病机制中发挥任何调节作用。方法用 GPR43 的特异性抗体标记人眼和小鼠眼,并用激光扫描共聚焦显微镜成像。在丁酸钠存在或不存在的情况下,用 TLR 配体刺激天真的 C57BL/6J (B6) 小鼠和 GPR43 基因敲除 (KO) 小鼠的角膜杯过夜,然后进行 RT-PCR 检测 GPR43 和细胞因子的表达。用 Poly I:C 诱导野生型(WT)B6、GPR43KO 和嵌合型小鼠患角膜炎,并通过角膜荧光素染色试验、浸润细胞染色和角膜整体装片计算来评估疾病的严重程度。丁酸盐能明显抑制几种 TLR 配体(如 Poly I:C、Flagellin 和 CpG-ODN,分别为 TLR-3、5 和 9 激动剂)在 WT 小鼠(而非 GPR43KO 小鼠)中引起的炎症。丁酸盐对 TLR 诱导的角膜炎的抑制作用是由组织细胞而非造血细胞中表达的 GPR43 介导的。SCFAs 可通过 GPR43 调节眼部炎症和免疫。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Short chain fatty acids inhibit corneal inflammatory responses to TLR ligands via the ocular G-protein coupled receptor 43

Purpose

Short chain fatty acids (SCFAs) produced by gut microbiota are known to play primary roles in gut homeostasis by immunomodulation partially through G-protein coupled receptors (GPR) 43. Using mouse models of TLR ligand induced keratitis, we investigated whether SCFAs and GPR43 play any regulatory roles in the pathogenesis of inflammatory responses in the eye.

Methods

Both human and mouse eyes were labeled with a specific antibody for GPR43 and imaged by a laser scanning confocal microscope. Corneal cups from naïve C57BL/6J (B6) and GPR43 knockout (KO) mice were stimulated with TLR ligands in the presence or absence of sodium butyrate overnight and then processed for RT-PCR assay for expression of GPR43 and cytokines. Keratitis was induced by Poly I:C in wild type (WT) B6, GPR43KO and chimeric mice and the disease severity was evaluated by the corneal fluorescein staining test, and infiltrating cell staining and calculating in corneal whole mount.

Results

GPR43 is expressed in both human and mouse eyes and the expression is bidirectionally regulated by TLR ligands and butyrate. Butyrate significantly inhibited inflammation caused by several TLR ligands such as Poly I:C, Flagellin, and CpG-ODN (TLR-3, 5 and 9 agonists, respectively) in WT, but not GPR43KO, mice. Butyrate inhibition of TLR-induced keratitis is mediated by the GPR43 expressed in tissue but not hematopoietic, cells.

Conclusions

This is the first report to demonstrate of the protective effect of SCFAs on microbial keratitis, and the dynamic expression and anti-inflammatory function of GPR43 in the eye. SCFAs can modulate inflammation and immunity in the eye through GPR43.

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来源期刊
Ocular Surface
Ocular Surface 医学-眼科学
CiteScore
11.60
自引率
14.10%
发文量
97
审稿时长
39 days
期刊介绍: The Ocular Surface, a quarterly, a peer-reviewed journal, is an authoritative resource that integrates and interprets major findings in diverse fields related to the ocular surface, including ophthalmology, optometry, genetics, molecular biology, pharmacology, immunology, infectious disease, and epidemiology. Its critical review articles cover the most current knowledge on medical and surgical management of ocular surface pathology, new understandings of ocular surface physiology, the meaning of recent discoveries on how the ocular surface responds to injury and disease, and updates on drug and device development. The journal also publishes select original research reports and articles describing cutting-edge techniques and technology in the field. Benefits to authors We also provide many author benefits, such as free PDFs, a liberal copyright policy, special discounts on Elsevier publications and much more. Please click here for more information on our author services. Please see our Guide for Authors for information on article submission. If you require any further information or help, please visit our Support Center
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