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Reversine attenuates cholestatic ductular reaction in rats

机译:逆转减弱大鼠胆汁淤积性导管反应

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Ductular reaction (DR) is usually observed in biliary disorders or various liver disorders, including nonalcoholic fatty liver disease. Few studies have focused on interrupting the DR process in the cholestatic environment. Here, we investigated the impact of reversine on DR in rats that had undergone bile duct ligation (BDL). Cholestatic injury was induced in rats 2 weeks following BDL. DR was assessed with biliary markers by immunohistochemistry. Biliary epithelial cells (BECs) were isolated for the analysis of proliferation and biliary factor gene expression. The effects of reversine on DR and fibrosis were analyzed in vivo via intraperitoneal injection in rats for 2 weeks. Chemically-induced BEC formation was used to investigate the biliary markers affected by reversine in vitro. DR with increased BEC expansion was identified in cholestatic liver injury, as indicated by CK7, CK19, and EpCAM expression around the portal vein in BDL rats. BDL-induced DR cells showed the increased expression of genes regulating cell proliferation (Ki67, Foxm1, and Pcna) and biliary markers (Krt7, Krt19, Epcam, Sox9, Cftr, and Asbt). Reversine attenuated cholestatic fibrosis and DR in rats. Reversine affected chemically-induced BEC formation, with the decreased expression of biliary Krt7, Cftr, and Ggt1 genes in vitro. BDL-induced Notch activation was attenuated upon reversine treatment in vivo, in part via the Notch/Sox9 pathway. In conclusion, reversine attenuated cholestatic ductular reaction and fibrosis in rats and reduced the bile duct formation associated with Dlk1/Notch/Sox9 signaling. Reversine may be regarded as a potential drug for cholangiopathies for preventing a ductular reaction.
机译:导管反应 (DR) 通常见于胆道疾病或各种肝脏疾病,包括非酒精性脂肪性肝病。很少有研究专注于中断胆汁淤积环境中的 DR 过程。在这里,我们研究了逆转对接受胆管结扎术 (BDL) 的大鼠 DR 的影响。BDL 后 2 周在大鼠中诱导胆汁淤积性损伤。DR 通过免疫组化用胆道标志物评估。分离胆道上皮细胞(BECs)用于增殖和胆道因子基因表达的分析。通过腹腔注射大鼠2周的体内分析逆转对DR和纤维化的影响。化学诱导的BEC形成用于研究受逆转作用的体外胆道标志物。如 BDL 大鼠门静脉周围的 CK7、CK19 和 EpCAM 表达所示,在胆汁淤积性肝损伤中发现了 BEC 扩增增加的 DR。BDL 诱导的 DR 细胞显示调节细胞增殖的基因(Ki67、Foxm1 和 Pcna)和胆道标志物(Krt7、Krt19、Epcam、Sox9、CFTR 和 Asbt)的表达增加。逆转减弱了大鼠胆汁淤积性纤维化和 DR。逆转影响化学诱导的 BEC 形成,胆汁 Krt7、Cftr 和 Ggt1 基因在体外表达降低。BDL 诱导的 Notch 激活在体内逆转处理后减弱,部分通过 Notch/Sox9 通路。总之,逆转减弱了大鼠的胆汁淤积性导管反应和纤维化,并减少了与 Dlk1/Notch/Sox9 信号相关的胆管形成。Reversine 可被视为治疗胆管病的潜在药物,用于预防导管反应。

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