Purification and characterization of liver cytochrome P-446 isolated from protein energy malnourished rats

Gil, Lionel; Vásquez, Hernán; Orellana, Miriam; Selkirk, James K.; Wold, Finn; Strobel, Henry W.

doi:10.1007/bf00229392

Cited by 1 publication

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“…It was concluded that nutritional status drastically changes the levels of some P-450 isozymes, providing an explanation for the observed changes in aryl hydrocarbon hydroxylase activity. More recently, Gil et a f . (1988) have purified to homogeneity and characterized a cytochrome P-450 isozyme from protein-energy malnourished rats induced with (3-naphthoflavone.…”

Section: Introductionmentioning

confidence: 97%

Nutrition‐related alterations in liver microsomal testosterone hydroxylases

et al. 1988

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The oxidation products of testosterone formed by liver microsomes from normal-fed and protein-energy malnourished male rats have been analysed by HPLC. Microsomes from normal-fed rats oxidized testosterone at a rate of 4.52 nmol/min/mg protein. The major products formed were: 6 beta-, 7 alpha- and 16-alpha-hydroxytestosterone; these three metabolites represented 65% of the total testosterone metabolism. Microsomes from protein-energy malnourished rats oxidized testosterone at a reduced rate of 2.03 nmol/min/mg protein. The major product formed was 7 alpha-hydroxytestosterone, which accounted for 43% of total testosterone oxidation. Microsomes from protein-energy malnourished rats showed a CO-reduced cytochrome P-450 spectra with a maxima at 452 nm, and a 38% decrease in the total content of cytochrome P-450. Some testosterone hydroxylases were drastically affected by protein-energy malnutrition but others, such as 7 alpha-hydroxylase, remained unchanged. The present results suggest that nutritional status can modify the relative amounts of individual cytochrome P-450 isozymes, thus explaining the observed changes in several testosterone hydroxylases. Protein-energy malnutrition seems to be an excellent tool with which to obtain a microsomal fraction containing predominantly P-450 isozymes, which are probably involved in key mono-oxygenations of physiological substrates.

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Section: Introductionmentioning

confidence: 97%