Decreased Ethanol Sensitivity and Tolerance Development in γ‐Protein Kinase C Null Mutant Mice Is Dependent on Genetic Background

Initial sensitivity and tolerance development to the sedative‐hypnotic and hypothermic effects of ethanol were investigated in γ‐protein kinase C (PKC) null mutant mice. Null mutants from a C57BL/6J × 129/SvJ mixed genetic background demonstrated decreased ethanol sensitivity and failed to develop chronic tolerance after 10 days of ethanol liquid diet. However, when the null mutation was introgressed onto a C57BL/6J background for six generations, the “no tolerance” phenotype for sedative‐hypnotic and hypothermic effects of ethanol was no longer apparent. Outcrossing the γ‐PKC null mutation to a C57BL/6J × 129/SvEvTac mixed background restored the “no tolerance” phenotype to ethanol‐induced sedation after chronic ethanol diet; however, as measured by hypothermia, tolerance was still evident in the null mutant mice. These observations and the results of tests of chronic tolerance in the C57BL/6J, 129/SvJ, and 129/SvEvTac background inbred strains indicate that γ‐PKC plays an important role in initial sensitivity and tolerance to ethanol. However, the impact of γ‐PKC is modulated by the background genotype. These results stress the importance of including the effect of genetic background when evaluating the effects of single gene mutations on quantitative behavioral traits.