Ethanol-induced CYP2E1 Expression is Reduced by Lauric Acid via PI3K Pathway in HepG2 Cells

Abstract: The metabolism of alcohol involves cytochrome P450 2E1 (CYP2E1)-induced oxidative stress, with the association of phosphatidylinositol-3-kinases (PI3K) and nuclear factor kappa B (NFκB) signalling pathways. CYP2E1 is primarily involved in the microsomal ethanol oxidising system, which generates massive reactive oxygen species (ROS) and ultimately leads to oxidative stress and tissue damage. Lauric acid, a major fatty acid in palm kernel oil, has been shown as a potential antioxidant. Here, we aimed to evaluate… Show more

“…The proteins involved in promoting various PTMs exist in several subcellular organelles, including the cytoplasm [39], ER [40,41], mitochondria [42], and nucleus [43]; PTMs may also be observed in the proteomes of the liver [37,[44][45][46][47], gut [7], and other peripheral tissues [29]. PTMs found in liver diseases include protein acetylation [37,42,48], nitration [10,26,37,[49][50][51][52][53], S-nitrosylation [49,54,55], oxidation [37], phosphorylation [26,56,57], succinylation [58], ADPribosylation [44], ubiquitination [37,59], SUMOylation [60][61][62][63][64][65], carbonylation [66][67][68], S-palmitoylation [45][46][47]69], gly...…”

“…The proteins involved in promoting various PTMs exist in several subcellular organelles, including the cytoplasm [ 39 ], ER [ 40 , 41 ], mitochondria [ 42 ], and nucleus [ 43 ]; PTMs may also be observed in the proteomes of the liver [ 37 , 44 – 47 ], gut [ 7 ], and other peripheral tissues [ 29 ]. PTMs found in liver diseases include protein acetylation [ 37 , 42 , 48 ], nitration [ 10 , 26 , 37 , 49 – 53 ], S -nitrosylation [ 49 , 54 , 55 ], oxidation [ 37 ], phosphorylation [ 26 , 56 , 57 ], succinylation [ 58 ], ADP-ribosylation [ 44 ], ubiquitination [ 37 , 59 ], SUMOylation [ 60 – 65 ], carbonylation [ 66 – 68 ], S -palmitoylation [ 45 – 47 , 69 ], glycosylation [ 7 , 37 , 70 , 71 ], protein adducts of aldehyde (i.e., acetaldehydes) [ 9 , 72 ], lipid peroxidation products (LPOs), and advanced glycation end products (AGEs) [ 6 , 66 , 74 – 79 ]. Several studies detail that specific PTMs correlate with exposures to excessive alcohol [ 80 , 81 ], CCl 4 [ 7 , 56 ], acetaminophen (APAP) [ 53 , 82 ], 3,4-methylenedioxymethamphetamine (MDMA, Ecstasy) [ 39 ], or fructose [ 51 ].…”

Contributing roles of mitochondrial dysfunction and hepatocyte apoptosis in liver diseases through oxidative stress, post-translational modifications, inflammation, and intestinal barrier dysfunction

“…The proteins involved in promoting various PTMs exist in several subcellular organelles, including the cytoplasm [39], ER [40,41], mitochondria [42], and nucleus [43]; PTMs may also be observed in the proteomes of the liver [37,[44][45][46][47], gut [7], and other peripheral tissues [29]. PTMs found in liver diseases include protein acetylation [37,42,48], nitration [10,26,37,[49][50][51][52][53], S-nitrosylation [49,54,55], oxidation [37], phosphorylation [26,56,57], succinylation [58], ADPribosylation [44], ubiquitination [37,59], SUMOylation [60][61][62][63][64][65], carbonylation [66][67][68], S-palmitoylation [45][46][47]69], gly...…”

“…The proteins involved in promoting various PTMs exist in several subcellular organelles, including the cytoplasm [ 39 ], ER [ 40 , 41 ], mitochondria [ 42 ], and nucleus [ 43 ]; PTMs may also be observed in the proteomes of the liver [ 37 , 44 – 47 ], gut [ 7 ], and other peripheral tissues [ 29 ]. PTMs found in liver diseases include protein acetylation [ 37 , 42 , 48 ], nitration [ 10 , 26 , 37 , 49 – 53 ], S -nitrosylation [ 49 , 54 , 55 ], oxidation [ 37 ], phosphorylation [ 26 , 56 , 57 ], succinylation [ 58 ], ADP-ribosylation [ 44 ], ubiquitination [ 37 , 59 ], SUMOylation [ 60 – 65 ], carbonylation [ 66 – 68 ], S -palmitoylation [ 45 – 47 , 69 ], glycosylation [ 7 , 37 , 70 , 71 ], protein adducts of aldehyde (i.e., acetaldehydes) [ 9 , 72 ], lipid peroxidation products (LPOs), and advanced glycation end products (AGEs) [ 6 , 66 , 74 – 79 ]. Several studies detail that specific PTMs correlate with exposures to excessive alcohol [ 80 , 81 ], CCl 4 [ 7 , 56 ], acetaminophen (APAP) [ 53 , 82 ], 3,4-methylenedioxymethamphetamine (MDMA, Ecstasy) [ 39 ], or fructose [ 51 ].…”

Contributing roles of mitochondrial dysfunction and hepatocyte apoptosis in liver diseases through oxidative stress, post-translational modifications, inflammation, and intestinal barrier dysfunction