Estradiol replacement enhances cocaine-stimulated locomotion in female C57BL/6 mice through estrogen receptor alpha

Psychostimulant effects are enhanced by ovarian hormones in women and female rodents. Estradiol increases behavioral responses to psychostimulants in women and female rats, although the underlying mechanism is unknown. This study utilized mice to investigate the time frame and receptor mediation of...

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Published in:Neuropharmacology 2013-09, Vol.72, p.236-249
Main Authors: Van Swearingen, Amanda E.D., Sanchez, Cristina L., Frisbee, Suzanne M., Williams, Antonia, Walker, Q. David, Korach, Kenneth S., Kuhn, Cynthia M.
Format: Article
Language:English
Subjects:
Analysis of Variance
Animals
Behavior
Cocaine
Cocaine - blood
Cocaine - pharmacology
Dopamine
Dopamine Uptake Inhibitors - pharmacology
Drug Interactions
Estradiol
Estradiol - pharmacology
Estrogen Receptor alpha - deficiency
Estrogen Receptor alpha - metabolism
Estrogen Receptor beta - deficiency
Estrogen Receptor beta - metabolism
Exploratory Behavior - drug effects
Female
Ginsenosides - pharmacology
Mice
Mice, Inbred C57BL
Mice, Knockout
Motor Activity - drug effects
NAD - pharmacology
Organ Size - drug effects
Ovariectomy
Sapogenins - pharmacology
Time Factors
Uterus - drug effects
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Summary:Psychostimulant effects are enhanced by ovarian hormones in women and female rodents. Estradiol increases behavioral responses to psychostimulants in women and female rats, although the underlying mechanism is unknown. This study utilized mice to investigate the time frame and receptor mediation of estradiol's enhancement of cocaine-induced behavior as mice enable parallel use of genetic, surgical and pharmacological methods. The spontaneous behavior of Sham and Ovariectomized (Ovx) female wildtype (WT) mice was determined during habituation to a novel environment and after cocaine administration. Ovx mice were replaced with vehicle (sesame oil) or 17β-estradiol (E2) for 2 days or 30 min prior to a cocaine challenge to investigate the time course of E2's effects. To examine receptor mediation of estradiol effects, Ovx mice replaced for 2 days with either the ERα-selective agonist PPT or the ERβ-selective agonist DPN were compared to Sham mice, and mice lacking either ERα (αERKO) or ERβ (βERKO) were compared to WT littermates. Ovx mice exhibited fewer ambulations during habituation than Sham females. Cocaine-induced increases in behavioral ratings were greater in Sham than in Ovx mice. Two days but not 30 min of E2 replacement in Ovx mice increased cocaine responses to Sham levels. PPT replacement also increased the cocaine response relative to vehicle- or DPN- treated Ovx mice. αERKO mice displayed modestly attenuated behavioral responses to novelty and cocaine compared to αWT littermates, but no behavioral differences were found between βERKO and βWT mice. These results suggest that E2 enhances cocaine-stimulated locomotion in mice predominantly through ERα. •Ovariectomy reduces cocaine-stimulated behavior in adult C57BL/6 mice.•Two day E2 treatment after ovariectomy enhances cocaine-stimulated locomotion.•Rapid E2 action over 30 min does not augment cocaine-stimulated locomotion.•Activation of ERα increases cocaine-stimulated locomotion in female mice.•Novelty- and cocaine-stimulated behaviors in female αERKOs are modestly reduced.
ISSN:0028-3908
1873-7064
DOI:10.1016/j.neuropharm.2013.04.015