CTGF公司
纤维化
癌症研究
信号转导
肺纤维化
医学
结缔组织
博莱霉素
肌成纤维细胞
免疫学
生物
生长因子
受体
内科学
病理
细胞生物学
化疗
作者
Jiani Liu,Zixin Pi,Yangfan Xiao,Zhuotong Zeng,Jiangfan Yu,Puyu Zou,Bingsi Tang,Xiangning Qiu,Rui Tang,Yaqian Shi,Rong Xiao
标识
DOI:10.1016/j.phrs.2022.106057
摘要
Systemic sclerosis (SSc) is a connective tissue disease with the involvement of complex signaling pathways, such as TGF-β/Smad2/3. SSc can lead to severe multiple organ fibrosis, but no effective therapy is currently available because of its unclear pathogenesis. Exploring new treatments is the focus of recent research on SSc. Recent studies have implied a potential antifibrotic role of esomeprazole (ESO), but with currently unidentified mechanisms. Signaling of AhR, a ligand-dependent transcription factor, has been described as a key controller of fibrosis, tumorigenesis, and immune balance. Recently, it has been reported that ESO may be an exogenous agonist of AhR signaling, while no previous study has revealed the effects of ESO on SSc and its underlying mechanisms. In this study, we demonstrate that ESO suppresses the migration of SSc dermal fibroblasts, downregulates profibrotic markers, including COLIA1, α-SMA CTGF and MMP1, and limits collagen production potentially via the activation of AhR signaling. More importantly, ESO could block Smad2/3 phosphorylation concurrently with the reduction in collagen via AhR signaling. Moreover, our results from the bleomycin (BLM)-induced SSc model in skin and lung shows that ESO ameliorates fibrosis in vivo, which in keeping with our in vitro results. We conclude that ESO is a potential therapeutic drug for SSc fibrosis.
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