MitoQ alleviates carbon tetrachloride-induced liver fibrosis in mice through regulating JNK/YAP pathway.

IF 2.2 4区 医学 Q3 TOXICOLOGY Toxicology Research Pub Date : 2022-10-01 DOI:10.1093/toxres/tfac062
Shulin Shan, Zhaoxiong Liu, Zhidan Liu, Cuiqin Zhang, Fuyong Song
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引用次数: 3

Abstract

Background: Liver fibrosis is a pathological wound-healing response caused by chronic liver damage. Mitochondria regulate hepatic energy metabolism and oxidative stress. Accumulating evidence has revealed that increased mitochondrial oxidative stress contributes to the activation of fibrogenesis. However, the roles and underlying mechanisms of mitochondrial oxidative stress in liver fibrosis remain unknown.

Methods and results: In this study, C57BL/6 mice were used to establish a model of liver fibrosis via oral gavage with CCl4 treatment for 8 weeks. Furthermore, intervention experiments were achieved by CCl4 combined with the intraperitoneal injection of mitoquinone mesylate (mitoQ). We demonstrated that the chronic CCl4 exposure resulted in severe hepatic fibrogenesis and significantly promoted the production of reactive oxygen species (ROS) and mitochondrial abnormalities. Besides, JNK/YAP pathway was also activated. By contrast, the administration of mitoQ markedly inhibited the expression of pro-fibrogenic transforming growth factor-β as well as type I collagen. The antifibrotic effects of mitoQ were also confirmed by hematoxylin and eosin staining and Sirius red staining. Moreover, mitoQ substantially reduced CCl4-induced mitochondrial damage and the release of ROS. Further studies suggested that this protection against liver fibrosis was mechanistically related to the inhibition of phosphorylation of JNK and the nuclear translocation of YAP.

Conclusion: In conclusion, these findings revealed that mitoQ attenuated liver fibrosis by inhibiting ROS production and the JNK/YAP signaling pathway. Selective targeting JNK/YAP may serve as a therapeutic strategy for retarding progression of chronic liver disease.

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MitoQ通过调控JNK/YAP通路减轻四氯化碳诱导的小鼠肝纤维化。
背景:肝纤维化是慢性肝损伤引起的病理性创面愈合反应。线粒体调节肝脏能量代谢和氧化应激。越来越多的证据表明,线粒体氧化应激的增加有助于纤维生成的激活。然而,线粒体氧化应激在肝纤维化中的作用和潜在机制尚不清楚。方法与结果:本研究采用C57BL/6小鼠,经CCl4灌胃治疗8周,建立肝纤维化模型。此外,CCl4联合腹腔注射甲磺酸米托醌(mitoQ)进行干预实验。我们证明慢性CCl4暴露导致严重的肝纤维化,并显著促进活性氧(ROS)的产生和线粒体异常。JNK/YAP通路也被激活。相比之下,给予mitoQ显著抑制促纤维化转化生长因子-β和I型胶原的表达。苏木精染色、伊红染色和天狼星红染色证实了mitoQ的抗纤维化作用。此外,mitoQ显著降低了ccl4诱导的线粒体损伤和ROS的释放。进一步的研究表明,这种对肝纤维化的保护作用与抑制JNK的磷酸化和YAP的核易位有关。结论:综上所述,这些发现揭示了mitoQ通过抑制ROS的产生和JNK/YAP信号通路来减轻肝纤维化。选择性靶向JNK/YAP可作为延缓慢性肝病进展的治疗策略。
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来源期刊
Toxicology Research
Toxicology Research TOXICOLOGY-
CiteScore
3.60
自引率
0.00%
发文量
82
期刊介绍: A multi-disciplinary journal covering the best research in both fundamental and applied aspects of toxicology
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