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Vol. 289, Issue 1, 54-65, April 1999
Laboratory for Developmental Neuroscience, Department of
Psychiatry, Albert Einstein College of Medicine, Bronx, New York
Evidence suggests the existence of genetic differences in cocaine
sensitization in male rats. The present study was undertaken to
investigate cocaine sensitization in female rats of genetically distinct inbred (Fischer 344 and Lewis) and outbred (Sprague-Dawley) strains. All female rats were bilaterally ovariectomized and randomly assigned to one of four experimental groups: 1) estradiol benzoate group, 2) progesterone group, 3) estradiol benzoate-plus-progesterone group, and 4) ovariectomized group. Additional controls included sham-operated female rats, female rats that received a single oil
injection, and female rats that received repeated oil injections. To
determine gender-related differences in the acute and chronic effects
of cocaine, data obtained from female rats were compared with those
from strain- and weight-matched male rats. Estradiol benzoate-plus-progesterone female rats showed greater locomotor effect
in response to an acute dose of cocaine and had more robust sensitization in response to repeated cocaine than did male rats. The
bilateral removal of ovaries abolished cocaine sensitization. In all
strains of rats studied, progesterone alone did not alter the
ovariectomy-induced attenuation of cocaine behavior, but estrogen alone
restored cocaine-induced behavioral sensitization. There were
significant strain effects on the degree of gonadal hormonal-induced modulation of cocaine sensitization in female rats. Female Lewis rats
were extremely sensitive to repeated-cocaine effects, whereas the
Fischer 344 female rats showed only marginal effects. The Sprague-Dawley rats ranked intermediate in their behavioral
sensitivity. The present study strongly supports the hypothesis that
female rats are more sensitive to both acute and chronic behavioral
effects of cocaine than are male rats and that the effects are strain dependent. It also shows that estrogen plays an important role in the
increased sensitivity of female rats to cocaine sensitization. Together, these data indicate significant interactions between ovarian
steroid hormones and genetic factors in cocaine-induced behavioral effects.
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