Pentoxifylline ameliorates non-alcoholic fatty liver disease in hyperglycaemic and dyslipidaemic mice by upregulating fatty acid β-oxidation

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作者
Jia-Hung Ye
Jung Chao
Ming-Ling Chang
Wen-Huang Peng
Hao-Yuan Cheng
Jiunn-Wang Liao
Li-Heng Pao
机构
[1] Research Center for Industry of Human Ecology,Division of Hepatology, Department of Gastroenterology and Hepatology
[2] College of Human Ecology,Department of Chinese Pharmaceutical Sciences and Chinese Medicine Resources
[3] Chang Gung University of Science and Technology,Department of Nursing
[4] Institute of Pharmacology,Department of Nutrition and Health Sciences
[5] College of Medicine,undefined
[6] National Yang-Ming University,undefined
[7] Liver Research Center,undefined
[8] Chang Gung Memorial Hospital,undefined
[9] College of Pharmacy,undefined
[10] China Medical University,undefined
[11] Chung Jen College of Nursing,undefined
[12] Health Sciences and Management,undefined
[13] Graduate Institute of Veterinary Pathology,undefined
[14] National Chung Hsing University,undefined
[15] Graduate Institute of Health-Industry Technology,undefined
[16] College of Human Ecology,undefined
[17] Chang Gung University of Science and Technology,undefined
[18] Chang Gung University of Science and Technology,undefined
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摘要
Nonalcoholic fatty liver disease (NAFLD), which includes simple steatosis, steatohepatitis, fibrosis, and cirrhosis, is characterised by abnormal fat accumulation in the liver in the absence of excessive alcohol intake. In patients with type 2 diabetes (T2D), concurrent NAFLD might increase the risk of chronic kidney disease and the mortality rate. Although several studies have examined the effectiveness of pentoxifylline (PTX) in NAFLD treatment, no results are available to verify the effectiveness of PTX in treating T2D associated with NAFLD. In this study, we developed a combined high-fat diet-induced obesity and low-dose streptozocin-induced hyperglycaemia mouse model to mimic the concurrent NAFLD and T2D pathological condition. By combining physiological assessments, pathological examinations, metabolomics studies on blood, urine, and liver, and measurements of gene and protein expression, we elucidated the effectiveness and the underlying mechanism of action of PTX in the hyperglycaemic and dyslipidaemic mice. Our results revealed that PTX ameliorated NAFLD in the hyperglycaemic and dyslipidaemic mice by upregulating fatty acid β-oxidation. Furthermore, the glycolysis pathway and branched-chain amino acid-related pathways in these mice were restored by PTX.
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