Effects of starvation on microsomal cytochrome P-450 and laurate-.OMEGA.-hydroxylation of rat kidney and liver.

Abstract Cytochrome P-450 (P-450) content and laurate-w-oxidation activity in rat kidney and liver microsomes were investigated following starvation. Multiple forms of P-450 were analyzed by one dimensional separation using peroxidase stained SDS-continuous gradient polyacrylamide gel electrophoresis. Gels of the hepatic microsomes treated with phenobarbital showed three P-450 bands, and the renal microsomes showed one sharp band, which was induced remarkably by starvation and coincided with the middle molecular form of P-450 from the hepatic microsomes. Since laurate-ω-oxidation activity was induced specifically by starvation but not by drug treatment, in both the kidney and the liver microsomes, the middle molecular form of P-450 might catalyze laurate-ω-oxidation. It seemed, therefore, that a special P-450 subunit catalyzing laurate-ω-oxidation has a greater function in the renal rather than hepatic microsomes because the specific laurate-ω-oxidation activity per starvation induced P-450 content was relatively similar in both the kidney and the liver.