FBLN1通过抑制TGF-β/Smad途径减少游离亚铁离子,从而调节急性呼吸窘迫综合征中的铁死亡。
FBLN1 regulates ferroptosis in acute respiratory distress syndrome by reducing free ferrous iron by inhibiting the TGF-β/Smad pathway.
作者信息
Yuan Yaping, Wang Youbo, Yan Yufeng, Kim Edward, Bai Jin, Zhao Yang, Ma Qinyun, Gu Wenchao, Song Haihan
机构信息
Department of Pulmonary and Critical Care Medicine, Shanghai Pudong New Area People's Hospital, Shanghai, China.
Department of Thoracic Surgery, Huashan Hospital, Fudan University, Shanghai, China.
出版信息
PLoS One. 2024 Dec 13;19(12):e0314750. doi: 10.1371/journal.pone.0314750. eCollection 2024.
BACKGROUND
Acute respiratory distress syndrome (ARDS) / acute lung injury (ALI) is a serious medical disease characterized by pulmonary dysfunction and inflammation. This study aims to determine the main molecular modules linked to ARDS and investigate the role of Fibulin-1 (FBLN1) in regulating ferroptosis in ARDS.
METHODS
Weighted Gene Co-expression Network Analysis (WGCNA) was employed on the GSE263867 dataset to find key modules associated with ALI. Differentially expressed genes (DEGs) and protein-protein interaction (PPI) networks were analyzed. MLE-12 cells were treated with lipopolysaccharide (LPS) to induce ferroptosis. In vitro studies were conducted to investigate the effects of FBLN1 and Transforming Growth Factor Beta 1 (TGF-β) overexpression on cell viability, oxidative stress markers, and ferroptosis-related proteins.
RESULTS
WGCNA identified the turquoise module as significantly negatively correlated with ARDS. Five key overlapping genes (GRIA1, OGN, COL14A1, FBLN1, and COL6A3) were significantly downregulated in ARDS samples. LPS treatment induced ferroptosis in MLE-12 cells, indicated by increased malondialdehyde (MDA), lipid reactive oxygen species (ROS), and ferrous iron (Fe2⁺) levels, and decreased cell viability and glutathione (GSH) levels. FBLN1 overexpression partially reversed these effects. Additionally, FBLN1 inhibited the TGF-β/Smad signaling pathway, as shown by decreased TGF-β and p-Smad protein levels. TGF-β overexpression exacerbated LPS-induced oxidative stress and ferroptosis, reducing cell viability and GSH levels. FBLN1 overexpression counteracted this effect, suggesting antagonistic roles for FBLN1 and TGF-β in regulating ferroptosis.
CONCLUSION
This study highlights FBLN1 as a critical regulator of ferroptosis in ARDS. Targeting the TGF-β/Smad pathway to modulate FBLN1 expression offers a potential therapeutic strategy to alleviate oxidative stress and mitigate pulmonary injury in inflammatory lung diseases.
背景
急性呼吸窘迫综合征(ARDS)/急性肺损伤(ALI)是一种以肺功能障碍和炎症为特征的严重医学疾病。本研究旨在确定与ARDS相关的主要分子模块,并研究纤连蛋白-1(FBLN1)在调节ARDS中铁死亡中的作用。
方法
对GSE263867数据集采用加权基因共表达网络分析(WGCNA)来寻找与ALI相关的关键模块。分析差异表达基因(DEG)和蛋白质-蛋白质相互作用(PPI)网络。用脂多糖(LPS)处理MLE-12细胞以诱导铁死亡。进行体外研究以探讨FBLN1和转化生长因子β1(TGF-β)过表达对细胞活力、氧化应激标志物和铁死亡相关蛋白的影响。
结果
WGCNA确定绿松石模块与ARDS显著负相关。五个关键重叠基因(GRIA1、OGN、COL14A1、FBLN1和COL6A3)在ARDS样本中显著下调。LPS处理诱导MLE-12细胞发生铁死亡,表现为丙二醛(MDA)、脂质活性氧(ROS)和亚铁离子(Fe2⁺)水平升高,细胞活力和谷胱甘肽(GSH)水平降低。FBLN1过表达部分逆转了这些作用。此外,FBLN1抑制TGF-β/Smad信号通路,表现为TGF-β和p-Smad蛋白水平降低。TGF-β过表达加剧了LPS诱导的氧化应激和铁死亡,降低了细胞活力和GSH水平。FBLN1过表达抵消了这种作用,表明FBLN1和TGF-β在调节铁死亡中具有拮抗作用。
结论
本研究强调FBLN1是ARDS中铁死亡的关键调节因子。靶向TGF-β/Smad途径调节FBLN1表达为减轻炎症性肺病中的氧化应激和减轻肺损伤提供了一种潜在的治疗策略。
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