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3,4-dihydroxytoluene,a metabolite of rutin,suppresses the progression of nonalcoholic fatty liver disease in mice by inhibiting p300 histone acetyltransferase activity

摘要3,3',4',5,7-Pentahydroxyflavone-3-rhamnoglucoside (rutin) is a flavonoid with a wide range of pharmacological activities.Dietary rutin is hardly absorbed because the microflora in the large intestine metabolize rutin into a variety of compounds including quercetin and phenol derivatives such as 3,4-dihydroxyphenolacetic acid (DHPAA),3,4-dihydroxytoluene (DHT),3,4-hydroxyphenylacetic acid (HPAA) and homovanillic acid (HVA).We examined the potential of rutin and its metabolites as novel histone acetyltransferase (HAT) inhibitors.DHPAA,HPAA and DHT at the concentration of 25 μM significantly inhibited in vitro HAT activity with DHT having the strongest inhibitory activity.Furthermore,DHT was shown to be a highly efficient inhibitor of p300 HAT activity,which corresponded with its high degree of inhibition on intracellular lipid accumulation in HepG2 cells.Docking simulation revealed that DHT was bound to the p300 catalytic pocket,bromodomain.Drug affinity responsive target stability(DARTS) analysis further supported the possibility of direct binding between DHT and p300.In HepG2 cells,DHT concentration-dependently abrogated p300-histone binding and induced hypoacetylation of histone subunits H3K9,H3K36,H4K8 and H4K16,eventually leading to the downregulation of lipogenesis-related genes and attenuating lipid accumulation.In ob/ob mice,administration of DHT (10,20 mg/kg,iv,every other day for 6 weeks) dose-dependently improved the NAFLD pathogenic features including body weight,liver mass,fat mass,lipid accumulation in the liver,and biochemical blood parameters,accompanied by the decreased mRNA expression of lipogenic genes in the liver.Our results demonstrate that DHT,a novel p300 histone acetyltransferase inhibitor,may be a potential preventive or therapeutic agent for NAFLD.

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作者 Jangho Lee [1] Ji-Hye Song [2] Min-Yu Chung [1] Jin-Hyuk Lee [3] Tae-Gyu Nam [4] Jae Ho Park [1] Jin-Taek Hwang [5] Hyo-Kyoung Choi [1] 学术成果认领
作者单位 Korea Food Research Institute,Jeollabuk-do 55365,Republic of Korea [1] Department of Biomedical Sciences,Asan Medical Center,University of Ulsan College of Medicine,Seoul 05505,Republic of Korea [2] Korea Research Institute of Bioscience and Biotechnology,Daejeon 34141,Republic of Korea;Department of Bioinformatics,Korea University of Science and Technology,Daejeon 34113,Republic of Korea [3] Major of Food Science and Biotechnology,Division of Bio-convergence,Kyonggi University,Suwon 16227,Republic of Korea [4] Korea Food Research Institute,Jeollabuk-do 55365,Republic of Korea;Department of Food Biotechnology,Korea University of Science and Technology,Daejeon 34113,Republic of Korea [5]
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发布时间 2021-09-28
基金项目
This study was supported by the Main Research Program (E-0150301) of the Korea Food Research Institute (KFRI)
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中国药理学报(英文版)

中国药理学报(英文版)

2021年42卷9期

1449-1460页

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