Fenofibrate alleviates NAFLD by enhancing the PPARα/PGC-1α signaling pathway coupling mitochondrial function.

IF 2.8 3区 医学 Q2 PHARMACOLOGY & PHARMACY BMC Pharmacology & Toxicology Pub Date : 2024-01-03 DOI:10.1186/s40360-023-00730-6
Xuemei Wang, Jieying Wang, Cao Ying, Yuan Xing, Xuan Su, Ke Men
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Abstract

Background: To comprehend the influences of fenofibrate on hepatic lipid accumulation and mitochondrial function-related signaling pathways in mice with non-alcoholic fatty liver disease (NAFLD) secondary to high-fat diets together with free fatty acids-influenced HepG2 cells model.

Materials and methods: A random allocation of male 6-week C57BL/6J mice into three groups was done, including controls, model (14 weeks of a high-fat diet), and fenofibrate [similar to the model one with administered 0.04 g/(kg.d) fenofibrate by gavage at 11 weeks for 4 weeks] groups, which contained 10 mice each. This study verified NAFLD pathogenesis via mitochondrial functions in hepatic pathological abnormalities, liver index and weight, body weight, serum biochemical indexes, oxidative stress indicators, mitochondrial function indexes, and related signaling pathways. The effect of fenofibrate intervention was investigated in NAFLD model mice. In vitro, four groups based on HepG2 cells were generated, including controls, the FFA model (1.5 mmol/L FFA incubation for 24 h), LV-PGC-1α intervention (similar to the FFA model one after PPARGC1A lentivirus transfection), and LV control intervention (similar to the FFA model one after negative control lentivirus transfection) groups. The study investigated the mechanism of PGC-1α related to lipid decomposition and mitochondrial biosynthesis by Oil red O staining, colorimetry and western blot.

Results: In vivo experiments, a high-fat diet achieved remarkable changes regarding liver weight, liver index, serum biochemical indicators, oxidative stress indicators, liver pathological changes, mitochondrial function indicators, and body weight of the NAFLD model mice while fenofibrate improved the objective indicators. In the HepG2 cells model, the lipid accumulation increased significantly within the FFA model group, together with aggravated hepatocytic damage and boosted oxidative stress levels. Moreover, FFA induced excessive mitosis into fragmented in mitochondrial morphology, ATP content in cells decreased, mtDNA replication fold decreased, the expression of lipid decomposition protein PPARα reduced, mitochondrial biosynthesis related protein PGC-1α, NRF-1 and TFAM decreased. PGC-1α overexpression inhibited lipid deposition by improving mitochondrial biosynthesis and lipid decomposition.

Conclusion: Fenofibrate up-regulated PPARα/PGC-1α signaling pathway, promoted mitochondrial β-oxidation, reduced oxidative stress damage and lipid accumulation of liver. PGC-1α overexpression enhanced mitochondrial biosynthesis and ATP production, and reduced HepG2 intracellular accumulation of lipids and oxidative stress.

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非诺贝特通过增强与线粒体功能耦合的 PPARα/PGC-1α 信号通路,缓解非酒精性脂肪肝。
背景:材料与方法:将6周龄雄性C57BL/6J小鼠随机分为三组,包括对照组、模型组(高脂饮食14周)和非诺贝特组(与模型组相似):将6周龄雄性C57BL/6J小鼠随机分为三组,包括对照组、模型组(高脂饮食14周)和非诺贝特组[与模型组相似,在11周时灌胃给药0.04 g/(kg.d)非诺贝特,连续4周],每组10只小鼠。该研究从肝脏病理异常、肝脏指数和重量、体重、血清生化指标、氧化应激指标、线粒体功能指标以及相关信号通路等方面验证了非酒精性脂肪肝通过线粒体功能致病的机制。非诺贝特干预对非酒精性脂肪肝模型小鼠的影响进行了研究。在体外,以HepG2细胞为基础产生了四组,包括对照组、FFA模型组(1.5 mmol/L FFA孵育24 h)、LV-PGC-1α干预组(PPARGC1A慢病毒转染后与FFA模型组相似)和LV对照干预组(阴性对照慢病毒转染后与FFA模型组相似)。研究通过油红 O 染色法、比色法和 Western 印迹法探讨了 PGC-1α 与脂质分解和线粒体生物合成相关的机制:在体内实验中,高脂饮食使非酒精性脂肪肝模型小鼠的肝脏重量、肝脏指数、血清生化指标、氧化应激指标、肝脏病理变化、线粒体功能指标和体重发生了显著变化,而非诺贝特则改善了这些客观指标。在 HepG2 细胞模型中,FFA 模型组的脂质积累显著增加,肝细胞损伤加重,氧化应激水平升高。此外,FFA诱导有丝分裂过度,导致线粒体形态破碎,细胞中ATP含量下降,mtDNA复制倍数减少,脂质分解蛋白PPARα表达减少,线粒体生物合成相关蛋白PGC-1α、NRF-1和TFAM表达减少。PGC-1α过表达可通过改善线粒体生物合成和脂质分解抑制脂质沉积:结论:非诺贝特能上调PPARα/PGC-1α信号通路,促进线粒体β氧化,减轻氧化应激损伤和肝脏脂质堆积。PGC-1α的过表达可增强线粒体的生物合成和ATP的产生,减少HepG2细胞内的脂质积累和氧化应激。
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来源期刊
BMC Pharmacology & Toxicology
BMC Pharmacology & Toxicology PHARMACOLOGY & PHARMACYTOXICOLOGY&nb-TOXICOLOGY
CiteScore
4.80
自引率
0.00%
发文量
87
审稿时长
12 weeks
期刊介绍: BMC Pharmacology and Toxicology is an open access, peer-reviewed journal that considers articles on all aspects of chemically defined therapeutic and toxic agents. The journal welcomes submissions from all fields of experimental and clinical pharmacology including clinical trials and toxicology.
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