Wang Jiahua, Zang Juan, Yu Yang, Liu Yang, Cao Huimin, Guo Ruibo, Zhang Lu, Liu Mo, Zhang Zixu, Li Xuetao, Kong Liang
College of Pharmacy, Liaoning University of Traditional Chinese Medicine, Dalian, China.
Key Laboratory of Ministry of Education for Traditional Chinese Medicine Viscera-State Theory and Applications, Liaoning University of Traditional Chinese Medicine, Shenyang, China.
Front Pharmacol. 2024 Aug 15;15:1426049. doi: 10.3389/fphar.2024.1426049. eCollection 2024.
The preservation of the Lingguizhugan (LGZG) decoction and patient compliance issue often limit the treatment of metabolic dysfunction-associated steatotic liver disease (MASLD). Hence, herein, an LGZG oral solution was developed for alleviating MASLD. Additionally, the potential mechanisms underlying LGZG-mediated MASLD mitigation were explored.
A MASLD mouse model was constructed using oleic and palmitic acid-induced LO2 cells and a high-fat diet. The apoptosis, lipid deposition, and mouse liver function were analyzed to assess the therapeutic effects of the LGZG oral solution on MASLD. Serum untargeted metabolomics, gut microbiota, bile acid (BA) metabolism, immunohistochemistry, and Western blotting analyses were performed to investigate the potential mechanism of action of LGZG oral solution on MASLD.
The LGZG oral solution ameliorated lipid deposition, oxidative stress, inflammation, and pathological damage. Serum untargeted metabolomics results revealed the LGZG-mediated regulation of the primary BA biosynthetic pathway. The 16S ribosomal RNA sequencing of the fecal microbiota showed that LGZG oral solution increased the relative abundance of the BA metabolism-associated , , and decreased that of . Additionally, the BA metabolism analysis results revealed a decrease in the total taurine-α/β-muricholic acid levels, whereas those of deoxycholic acid were increased, which activated specific receptors in the liver and ileum, including farnesoid X receptor (FXR) and takeda G protein-coupled receptor 5 (TGR5). Activation of FXR resulted in an increase in short heterodimer partner and subsequent inhibition of cholesterol 7α-hydroxylase and sterol regulatory element-binding protein-1c expression, and activation of FXR also results in the upregulation of fibroblast growth factor 15/19 expression, and consequently inhibition of cholesterol 7α-hydroxylase, which correlated with hepatic BA synthesis and lipogenesis, ultimately attenuating lipid deposition and bile acid stasis, thereby improving MASLD.
Altogether, the findings of this study suggest that modulating microbiota-BA-FXR/TGR5 signaling pathway may be a potential mechanism of action of LGZG oral solution for the treatment of MASLD.
苓桂术甘汤(LGZG)的保存及患者依从性问题常限制代谢功能障碍相关脂肪性肝病(MASLD)的治疗。因此,本文研制了一种LGZG口服溶液用于缓解MASLD。此外,还探讨了LGZG介导减轻MASLD的潜在机制。
利用油酸和棕榈酸诱导LO2细胞并结合高脂饮食构建MASLD小鼠模型。分析细胞凋亡、脂质沉积及小鼠肝功能,以评估LGZG口服溶液对MASLD的治疗效果。进行血清非靶向代谢组学、肠道微生物群、胆汁酸(BA)代谢、免疫组织化学和蛋白质印迹分析,以研究LGZG口服溶液对MASLD作用的潜在机制。
LGZG口服溶液改善了脂质沉积、氧化应激、炎症和病理损伤。血清非靶向代谢组学结果显示LGZG介导了初级BA生物合成途径的调节。粪便微生物群的16S核糖体RNA测序表明,LGZG口服溶液增加了与BA代谢相关的[具体菌属1]、[具体菌属2]、[具体菌属3]的相对丰度,并降低了[具体菌属4]的相对丰度。此外,BA代谢分析结果显示总牛磺酸-α/β-鼠胆酸水平降低,而脱氧胆酸水平升高,这激活了肝脏和回肠中的特定受体,包括法尼醇X受体(FXR)和武田G蛋白偶联受体5(TGR5)。FXR的激活导致短异源二聚体伴侣增加,随后抑制胆固醇7α-羟化酶和甾醇调节元件结合蛋白-1c的表达,FXR的激活还导致成纤维细胞生长因子15/19表达上调,从而抑制胆固醇7α-羟化酶,这与肝脏BA合成和脂肪生成相关,最终减轻脂质沉积和胆汁酸淤积,从而改善MASLD。
总之,本研究结果表明,调节微生物群-BA-FXR/TGR5信号通路可能是LGZG口服溶液治疗MASLD的潜在作用机制。
