1970
DOI: 10.1159/000458360
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Metabolism of Ethanol and Fructose in the Perfused Rat Liver

Abstract: Ethanol utilization by the isolated perfused rat liver was studied under various experimental conditions. 1. A linear decrease of the ethanol concentration in the perfusing medium was observed, indicating that ethanol utilization was independent of the ethanol concentration. 2. Inhibition of alcohol dehydrogenase by pyrazol was paralleled by a decrease in ethanol utilization. 3. The uptake of fructose and its conversion to glucose were inhibited by ethanol. Ethanol utilization was diminished in the presence of… Show more

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Cited by 57 publications
(7 citation statements)
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“…2. The data, therefore, disprove the notion that fructose has no effect on ethanol metabolism in rat liver [49]. The stimulation was dependent on the ethanol concentration; and glycerol (A-A).…”
Section: Stimulution Of Ethanol Oxidation By Fructosementioning
confidence: 48%
“…2. The data, therefore, disprove the notion that fructose has no effect on ethanol metabolism in rat liver [49]. The stimulation was dependent on the ethanol concentration; and glycerol (A-A).…”
Section: Stimulution Of Ethanol Oxidation By Fructosementioning
confidence: 48%
“…3). In addition to our general knowledge concerning ethanol oxidation in the liver by ADH and Acetaldehyd-dehydrogenase (17, 39), the limiting significance of NADH 2 reoxidation for ethanol degradation in the liver (21, 36)$ the increased NADH2/ NAD quotient of various redox systems, e. g. lactate-pyruvate, L-I-Glycerophosphate-dihydroxyacetonphosphate, are well known (2,11,12,28,41). L-Iglycerophosphate is the only FFA acceptor in the triglyceride synthesis.…”
Section: --mentioning
confidence: 99%
“…The metabolism of ethanol can be catalyzed in vitro by various enzymes including alcohol dehydrogenase (ADH) [30,43], the microsomal ethanol-oxidizing sys tem (MEOS) [ The present study was undertaken to in vestigate the effect of testosterone, estradiol and castration on MEOS activity of livers derived from mature male rats. In addition, the data were compared with the microsomal content of cytochrome P-450 and the activi ties of microsomal NADPH-cytochrome c reductase as well as other hepatic alcoholmetabolizing enzymes.…”
Section: Introductionmentioning
confidence: 99%