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非瑟酮通过抑制 NCOA4 介导体细胞铁死亡缓解博来霉素诱导的特发性肺纤维化。

Fraxetin alleviates BLM-induced idiopathic pulmonary fibrosis by inhibiting NCOA4-mediated epithelial cell ferroptosis.

机构信息

Department of Basic Medicine, Wuxi School of Medicine, Jiangnan University, Wuxi, 214122, Jiangsu, China.

School of Life Sciences and Health Engineering, Jiangnan University, Wuxi, 214122, Jiangsu, China.

出版信息

Inflamm Res. 2023 Nov;72(10-11):1999-2012. doi: 10.1007/s00011-023-01800-5. Epub 2023 Oct 5.

DOI:10.1007/s00011-023-01800-5
PMID:37798541
Abstract

INTRODUCTION

Idiopathic pulmonary fibrosis (IPF) is a debilitating lung condition with few available treatments. The early driver of wound repair that contributes to IPF has been extensively identified as repetitive alveolar epithelial damage. According to recent reports, IPF is linked to ferroptosis, a unique type of cell death characterized by a fatal buildup of iron and lipid peroxidation.

OBJECTIVE AND METHOD

There is little information on epithelial cells that induce pulmonary fibrosis by going through ferroptosis. In this study, we used bleomycin (BLM) to examine the impact of ferroptosis on IPF in mouse lung epithelial cells (MLE-12).

RESULTS

We discovered that BLM increases ferroptosis in MLE-12. Additionally, we found that NCOA4 is overexpressed and plays a key role in the ferroptosis of epithelial cells throughout the IPF process. Using Molecular docking, we found that Fraxetin, a natural component extracted from Fraxinus rhynchophylla, formed a stable binding to NCOA4. In vitro investigations showed that Fraxetin administration greatly decreased ferroptosis and NCOA4 expression, which in turn lowered the release of inflammatory cytokines.

CONCLUSION

Fraxetin treatment significantly alleviated BLM-induced lung inflammation and fibrosis. Our findings imply that fraxetin possesses inhibitory roles in ferroptosis and can be a potential drug against IPF.

摘要

简介

特发性肺纤维化(IPF)是一种使人虚弱的肺部疾病,目前可用的治疗方法很少。导致 IPF 的早期伤口修复驱动因素已被广泛确定为反复的肺泡上皮损伤。根据最近的报告,IPF 与铁死亡有关,铁死亡是一种独特的细胞死亡类型,其特征是铁和脂质过氧化的致命积累。

目的和方法

关于通过铁死亡诱导肺纤维化的上皮细胞的信息很少。在这项研究中,我们使用博来霉素(BLM)来检查铁死亡对小鼠肺上皮细胞(MLE-12)中 IPF 的影响。

结果

我们发现 BLM 增加了 MLE-12 中的铁死亡。此外,我们发现 NCOA4 过表达,并在整个 IPF 过程中上皮细胞的铁死亡中发挥关键作用。通过分子对接,我们发现从秦皮中提取的天然成分 Fraxetin 与 NCOA4 形成稳定的结合。体外研究表明,Fraxetin 给药可显著降低铁死亡和 NCOA4 表达,进而降低炎症细胞因子的释放。

结论

Fraxetin 治疗可显著减轻 BLM 诱导的肺炎症和纤维化。我们的研究结果表明,Fraxetin 具有抑制铁死亡的作用,可能是治疗 IPF 的潜在药物。

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