齐多夫定通过促进脂肪酸氧化改善高脂饮食诱导的大鼠代谢紊乱OA
Zidovudine ameliorates metabolic disorders in HFD-fed rats by enhancing fatty acid oxidation
探讨齐多夫定(AZT)对高脂饮食(HFD)诱导大鼠代谢紊乱的改善作用及其潜在机制.通过建立 HFD大鼠模型,设置正常对照组、模型组及 AZT低剂量(25 mg/kg)和高剂量(50 mg/kg)干预组,评价 AZT对代谢表型、肝脏脂质沉积、氧化应激、线粒体功能以及过氧化物酶体增殖物激活受体(PPAR)信号通路的影响.结果显示,与模型组相比,AZT显著抑制体重增长,降低腹股沟白色脂肪组织及附睾白色脂肪组织的重量和细胞体积,增强代谢灵活性,并改善葡萄糖耐量且不引起血乳酸升高.高剂量 AZT能进一步降低肝脏甘油三酯水平,减轻脂肪变性,并通过提高超氧化物歧化酶(SOD)活性、降低丙二醛(MDA)水平以缓解肝脏氧化应激.蛋白免疫印迹实验结果显示,AZT可上调肝脏 PPARα及肉碱棕榈酰转移酶 1α(CPT1α)蛋白表达,下调 PPARγ表达.综上,AZT能有效改善 HFD诱导的代谢紊乱且未引起线粒体毒性,其作用可能与促进脂肪酸氧化、减轻氧化应激、调控PPAR通路和嘧啶代谢有关.
This study aimed to investigate the effects of zidovudine(AZT)on high-fat diet(HFD)-induced metabolic disturbances in rats and its underlying mechanisms.The HFD rat model was established,and the animals were divided into the control group,the model group,and the AZT-treated group at low(25 mg/kg)and high(50 mg/kg)doses.Metabolic phenotype,hepatic lipid deposition,oxidative stress,mitochondrial function,and peroxisome proliferator-activated receptor(PPAR)signaling were evaluated.AZT treatment significantly mitigated HFD-induced body weight gain and reduced both the mass and adipocyte size of inguinal and epididymal white adipose tissues;it also enhanced metabolic flexibility and improved glucose tolerance without elevating blood lactate levels.High-dose AZT further lowered hepatic triglyceride accumulation,ameliorated steatosis,and additionally,attenuated hepatic oxidative stress by increasing superoxide dismutase(SOD)activity and decreasing malondialdehyde(MDA)levels.Western blot analysis revealed that AZT upregulated hepatic PPARα and carnitine palmitoyltransferase 1α(CPT1α),while downregulating PPARγ expression.In conclusion,A ZT effectively ameliorates HFD-induced metabolic disorders without inducing mitochondrial toxicity,which may be related to the promotion of fatty acid oxidation,the reduction of oxidative stress,and the modulation of both the PPAR signaling pathway and pyrimidine metabolism.
张靖;金子爱;王紫悦;林君谦;王涛
中国药科大学多靶标天然药物全国重点实验室新药筛选中心,南京 210009||江苏省药效研究与评价服务中心,南京 210009中国药科大学多靶标天然药物全国重点实验室新药筛选中心,南京 210009||江苏省药效研究与评价服务中心,南京 210009中国药科大学多靶标天然药物全国重点实验室新药筛选中心,南京 210009||江苏省药效研究与评价服务中心,南京 210009中国药科大学多靶标天然药物全国重点实验室新药筛选中心,南京 210009||江苏省药效研究与评价服务中心,南京 210009中国药科大学多靶标天然药物全国重点实验室新药筛选中心,南京 210009||江苏省药效研究与评价服务中心,南京 210009
医药卫生
齐多夫定高脂饮食代谢紊乱脂肪酸氧化氧化应激线粒体功能PPAR信号通路
zidovudinehigh-fat dietmetabolic disorderfatty acid oxidationoxidative stressmitochondrial functionPPAR signaling pathway
《中国药科大学学报》 2026 (2)
256-265,10
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