Abstract

We set out to find if the strain-specific, male-specific hepatic expression of Cyp4a protein in mouse was due to expression of Cyp4a12 and to understand the genetic basis for reported differences in expression. 12-Lauric acid hydroxylase (LAH) activity was found to show higher levels in male ddY, but not C57Bl/6, mouse liver microsomes. The expression of Cyp4a12 mRNA was studied using RNAase protection assays in male and female liver and kidney of nine mouse strains. Cyp4a12 was found to be highly expressed in male liver and kidney, but at much lower levels in female liver and kidney, in all strains studied. Western blotting with an antibody specific for Cyp4a12 confirmed that Cyp4a12 was expressed in a male specific fashion in C57Bl/6 mouse liver. RNAase protection analysis for Cyp4a10 and 14 in ddY mice revealed that neither of these genes showed male-specific expression. To further investigate genetic factors that control male-specific Cyp4a12 expression, PPARα+/+ and −/− mice were studied, showing that total P450 and 12-LAH activity was male-specific in +/+, but not −/− mice. RNAase protection assays were used to confirm that Cyp4a12 was lower in −/− mice. However, the male-specific Slp and MUP-1 genes retained hepatic male-specific levels of expression in +/+ and −/− mice, showing that the decrease in Cyp4a12 was not a general effect on male-specific expression. Thus, PPARα has a specific effect on constitutive expression of Cyp4a12.

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