Duloxetine enhances PAX6 expression and suppresses innate immune responses in murine LPS-induced corneal inflammation

IF 5.9 1区 医学 Q1 OPHTHALMOLOGY Ocular Surface Pub Date : 2024-08-08 DOI:10.1016/j.jtos.2024.08.008
Petros Moustardas , Mojdeh Abbasi , Dina Javidjam , Cindy Saah Asamoah , Arnaud Schweitzer-Chaput , Salvatore Cisternino , Dominique Bremond-Gignac , Daniel Aberdam , Neil Lagali
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Abstract

Background-aim

PAX6 is a key regulator of eye development and epithelial homeostasis in the cornea. When deficient, chronic corneal inflammation, neovascularization and limbal stem cell deficiency can occur. Here we investigated the potential of duloxetine, a generic serotonin reuptake inhibitor that can upregulate PAX6 in vitro, for its in vivo activity in the context of corneal inflammation.

Methods

Duloxetine tolerance was tested in a human limbal stem cell line and isogenic CRISPR-knockout PAX6+/− cells. C57BL/6-Wildtype mice were administered duloxetine eye drops at concentrations of 1 μM - 2 mM and tested for toxicity and corneal PAX6 expression. In LPS-induced corneal inflammation in mice, duloxetine's effect on PAX6 expression, corneal opacification and inflammatory responses were evaluated by in vivo corneal imaging, immunostaining, and whole-transcriptome microarray analysis.

Results

No toxicity was observed in vitro for duloxetine concentrations up to 10μΜ. In vivo, duloxetine drops were well-tolerated up to 50 μM. Duloxetine drops at 10μΜ significantly upregulated PAX6 protein levels in the cornea by 30 % within 2 days. In the LPS model, duloxetine resulted in a sustained 33 % PAX6 protein upregulation in the cornea at 7 days, and in reduced opacity within 2 days, accompanied by a significant dampening of IL-17A signaling, neutrophil degranulation, microglial activation, macrophage markers, and MMP expression, despite non-significant changes in total inflammatory cell infiltration.

Conclusion

Short-term administration of a repurposed generic drug, duloxetine, upregulates PAX6 protein levels in the cornea of mice and exerts an anti-inflammatory activity by dampening innate immune responses.

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度洛西汀能增强 PAX6 的表达,并抑制 LPS 诱导的小鼠角膜炎症中的先天性免疫反应。
背景-目的:PAX6 是眼睛发育和角膜上皮稳态的关键调节因子。当PAX6缺乏时,会出现慢性角膜炎症、新生血管和角膜缘干细胞缺乏症。杜洛西汀是一种普通的血清素再摄取抑制剂,可在体外上调 PAX6,我们在此研究了其在角膜炎症中的体内活性潜力:方法:在人类角膜缘干细胞系和同源 CRISPR 基因敲除 PAX6+/- 细胞中测试度洛西汀耐受性。给 C57BL/6 野生型小鼠滴入浓度为 1μM - 2mM 的度洛西汀眼药水,并测试其毒性和角膜 PAX6 表达。在 LPS 诱导的小鼠角膜炎中,通过体内角膜成像、免疫染色和全转录组芯片分析,评估了度洛西汀对 PAX6 表达、角膜翳和炎症反应的影响:结果:在体外,度洛西汀浓度达到10μΜ时未观察到毒性。在体内,度洛西汀滴剂的耐受性高达 50μM。10μΜ的度洛西汀滴眼液可在2天内使角膜中的PAX6蛋白水平显著提高30%。在LPS模型中,度洛西汀可使角膜中的PAX6蛋白水平在7天内持续上调33%,并在2天内降低角膜翳,同时显著抑制IL-17A信号传导、中性粒细胞脱颗粒、小胶质细胞活化、巨噬细胞标志物和MMP表达,尽管炎症细胞浸润总量无明显变化:结论:短期服用一种再利用的普通药物度洛西汀可上调小鼠角膜中的 PAX6 蛋白水平,并通过抑制先天性免疫反应发挥抗炎活性。
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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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