Hua Xie, Zhongxian Zhu, Jiaqi Tang, Wei Zhu, Mengyan Zhu, Amy Wing Yi Wai, Junzhi Li, Zhongluan Wu, Paul Kwong Hang Tam, Vincent Chi Hang Lui, Weibing Tang
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Oxidative stress in human intrahepatic biliary epithelial cells transfected with a constitutively active YAP1 (YAPS127A) plasmid was assessed using quantitative reverse transcriptase-PCR and fluorescence-activated cell sorting analysis. PRDX1 expression in BA and experimental BA mouse model livers was examined by double immunofluorescence. The mRNA expression and nuclear localization of YAP1 in EpCAM-expressing bile duct cells were increased in the livers of BA and experimental BA mouse model. Aberrant development of intrahepatic organoids, differential expression of oxidative stress response genes Sod3 and Prdx1, enrichment of oxidative stress, and mitochondrial reactive oxidative stress-associated gene sets were observed in organoids treated with the Hippo-YAP1 activator, whereas organoid development was unaffected by the addition of the Hippo-YAP1 inhibitor. Transfection with constitutively active YAP1 led to the downregulation of PRDX1 and oxidative stress in human intrahepatic biliary epithelial cells. Additionally, reduced PRDX1 expression was also observed in the bile duct of human BA and experimental BA mouse livers. In conclusion, dysregulated activation of Hippo-YAP1 signaling induces oxidative stress and impairs the development of intrahepatic biliary organoids, which indicates therapeutic strategies targeting Hippo-YAP1 signaling may offer the potential to improve biliary repair and regeneration in patients with BA.</p>","PeriodicalId":17930,"journal":{"name":"Laboratory Investigation","volume":" ","pages":"102199"},"PeriodicalIF":5.1000,"publicationDate":"2024-11-22","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Dysregulated Activation of Hippo-YAP1 Signaling Induces Oxidative Stress and Aberrant Development of Intrahepatic Biliary Cells in Biliary Atresia.\",\"authors\":\"Hua Xie, Zhongxian Zhu, Jiaqi Tang, Wei Zhu, Mengyan Zhu, Amy Wing Yi Wai, Junzhi Li, Zhongluan Wu, Paul Kwong Hang Tam, Vincent Chi Hang Lui, Weibing Tang\",\"doi\":\"10.1016/j.labinv.2024.102199\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>The canonical Hippo-YAP1 signaling pathway is crucial for liver development and regeneration, but its role in repair and regeneration of intrahepatic bile duct in biliary atresia (BA) remains largely unknown. 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引用次数: 0
摘要
典型的Hippo-YAP1信号通路对肝脏的发育和再生至关重要,但它在胆道闭锁(BA)肝内胆管的修复和再生中的作用在很大程度上仍然未知。本研究采用定量反转录酶-PCR(qRT-PCR)和双重免疫荧光技术检测了YAP1在胆道闭锁患者肝组织和恒河猴轮状病毒(RRV)诱导的实验性胆道闭锁小鼠模型中的表达。生成小鼠 EpCAM 表达细胞衍生的肝脏器官组织,并用 Hippo-YAP1 通路激活剂(Xmu-mp-1 和 TRULI)或抑制剂(Peptide17)处理。研究人员进行了形态学、免疫荧光、RNA-seq和生物信息学分析。利用 qRT-PCR 和荧光激活细胞分选分析评估了转染了组成型活性 YAP1(YAPS127A)质粒的人肝内胆管上皮细胞(HiBECs)的氧化应激。通过双重免疫荧光检测了 BA 和实验性 BA 小鼠模型肝脏中 PRDX1 的表达。在 BA 和实验性 BA 小鼠模型肝脏中,表达 EpCAM 的胆管细胞中 YAP1 的 mRNA 表达和核定位增加。在使用Hippo-YAP1激活剂处理的器官组织中,观察到肝内器官组织发育异常、氧化应激反应基因Sod3和Prdx1的差异表达、氧化应激和线粒体反应性氧化应激(mito-ROS)相关基因组的富集,而加入Hippo-YAP1抑制剂后器官组织的发育不受影响。转染组成型活性 YAP1 会导致 PRDX1 下调和 HiBECs 中的氧化应激。此外,在人类 BA 和实验性 BA 小鼠肝脏的胆管中也观察到了 PRDX1 表达的降低。总之,Hippo-YAP1 信号的失调激活会诱导氧化应激并损害肝内胆道器官组织的发育,这表明针对 Hippo-YAP1 信号的治疗策略可能会改善 BA 患者的胆道修复和再生。
Dysregulated Activation of Hippo-YAP1 Signaling Induces Oxidative Stress and Aberrant Development of Intrahepatic Biliary Cells in Biliary Atresia.
The canonical Hippo-YAP1 signaling pathway is crucial for liver development and regeneration, but its role in repair and regeneration of intrahepatic bile duct in biliary atresia (BA) remains largely unknown. YAP1 expression in the liver tissues of patients with BA and Rhesus rotavirus-induced experimental BA mouse models were examined using quantitative reverse transcriptase-PCR and double immunofluorescence. Mouse EpCAM-expressing cell-derived liver organoids were generated and treated with Hippo-YAP1 pathway activators (Xmu-mp-1 and TRULI) or an inhibitor (Peptide17). Morphologic, immunofluorescence, RNA-seq, and bioinformatic analyses were performed. Oxidative stress in human intrahepatic biliary epithelial cells transfected with a constitutively active YAP1 (YAPS127A) plasmid was assessed using quantitative reverse transcriptase-PCR and fluorescence-activated cell sorting analysis. PRDX1 expression in BA and experimental BA mouse model livers was examined by double immunofluorescence. The mRNA expression and nuclear localization of YAP1 in EpCAM-expressing bile duct cells were increased in the livers of BA and experimental BA mouse model. Aberrant development of intrahepatic organoids, differential expression of oxidative stress response genes Sod3 and Prdx1, enrichment of oxidative stress, and mitochondrial reactive oxidative stress-associated gene sets were observed in organoids treated with the Hippo-YAP1 activator, whereas organoid development was unaffected by the addition of the Hippo-YAP1 inhibitor. Transfection with constitutively active YAP1 led to the downregulation of PRDX1 and oxidative stress in human intrahepatic biliary epithelial cells. Additionally, reduced PRDX1 expression was also observed in the bile duct of human BA and experimental BA mouse livers. In conclusion, dysregulated activation of Hippo-YAP1 signaling induces oxidative stress and impairs the development of intrahepatic biliary organoids, which indicates therapeutic strategies targeting Hippo-YAP1 signaling may offer the potential to improve biliary repair and regeneration in patients with BA.
期刊介绍:
Laboratory Investigation is an international journal owned by the United States and Canadian Academy of Pathology. Laboratory Investigation offers prompt publication of high-quality original research in all biomedical disciplines relating to the understanding of human disease and the application of new methods to the diagnosis of disease. Both human and experimental studies are welcome.
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