Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
8548529 | Food and Chemical Toxicology | 2018 | 8 Pages |
Abstract
Green tea and (-)-epigallocatechin-3-gallate (EGCG) have been studied for their obesity-related health effects. Many green tea extract (GTE)-based dietary supplements are commercially-available. Although green tea beverage has a long history of safe use, a growing number of case-reports have linked GTE-based supplements to incidents of hepatotoxicity. Animal studies support the hepatotoxic potential of GTE and EGCG, but the mechanisms remain unclear. Here, we examined the hepatotoxic effects of EGCG in C57BL/6J mice and evaluated changes in hepatic antioxidant response and mitochondria structure and function. Intragastric dosing with EGCG (500 - 750 mg/kg) once daily for 3 d caused hepatic inflammation, necrosis, and hemorrhage. Hepatotoxicity was associated with increased oxidative stress and decreased superoxide dismutase and glutathione peroxidase levels. Real-time PCR and transmission electron microscopy showed decreased hepatic mitochondria copy number in EGCG-treated mice. The mRNA levels of marker genes of respiratory complex I and III, sirtuin 3, forkhead box O3a, and peroxisome-EGCG-treated mice. Sirtuin 3 protein levels were also decreased by EGCG. Our data indicate the mitochondria may be a target for EGCG, and that inhibition of mitochondria function/antioxidant response may be important for the hepatotoxicity of bolus EGCG.
Keywords
FOXO3aMT-CO2Rps18MDACytochrome oxidase subunit II(-)-Epigallocatechin-3-gallatephosphorylated histone 2AXSirtuin 3PGC1αGPx1γH2AXSirt3SOD2HPLC-ECDGSHEGCGGAPDHALTqRT-PCRqPCRQuantitative PCRASTAspartate aminotransferaseAlanine aminotransferaseTemOxidative stressforkhead box O3aHepatotoxicitymalondialdehydeMitochondriaTransmission electron microscopyGreen teareduced glutathionehigh performance liquid chromatography with electrochemical detectionglutathione peroxidase 1glyceraldehyde-3 phosphate dehydrogenase
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Authors
Karma D. James, Mary J. Kennett, Joshua D. Lambert,