The Effects of Selective Estrogenic Drugs in the Medial Amygdala on Male Rat Sexual Behavior

Ogaga-Mgbonyebi, Ejiroghene V.

15 December 2010

Male rat copulatory behavior is dependent on Testosterone (T) and its metabolites, estradiol (E2) and dihydrotestosterone (DHT). The estrogen receptor (ER) isoforms, ERα and ERβ, exist in the medial Amygdala (MEA) and either receptor might mediate mating behavior. Therefore, the effects of selective estrogenic MEA implants: propyl pyrazole triol (PPT, ERα agonist), diarylpropionitrile (DPN, ERβ agonist), and 1-methyl-4-phenyl pyridinium (MPP, ERα antagonist) were compared to E2 in maintaining sexual behavior. Four groups of male rats were castrated and administered DHT s.c. and bilateral MEA implants containing either cholesterol, E2, PPT or DPN. An additional group of gonadally intact male rats received bilateral MPP-MEA implants. The post-surgical trials showed a significant decrease in the mating behavior of groups that received cholesterol, PPT, or DPN-MEA implants. However, sexual behavior was maintained in male rats that received the E2 or MPP-MEA implants. These results suggest a differential response of the MEA to E2.

Estradiol

Estrogen receptor

Medial amygdala

Sexual behavior

Propyl pyrazole triol

Biology, general

Implant of a Selective Estrogen Receptor Alpha Agonist to the Male Rat Medial Preoptic Area Maintains Mating Behavior

Habteab, Biniyam Seged

02 May 2007

ABSTRACT Evidence from knockout studies in male mice and from experiments in male rats,in which expression of the estrogen receptor alpha (ERα) gene was inhibited in the medial preoptic area (MPO), suggests that ERα is important in the control of male rat mating behavior. Therefore, in this experiment, we tested the hypothesis that activation of ERα in the MPO is sufficient to maintain mating behavior in castrated male rats receiving subcutaneously (s.c.) dihydrotestosterone (DHT), a non-aromatizable androgen. Accordingly, castrated rats treated with DHT s.c. received MPO implants of either: (i) propyl-pyrazole-triol (PPT) (Stauffer, et al 2000; Katzenellenbogen, et al 2000), a selective ERα agonist, (ii) E2 (positive controls) or (iii) cholesterol (negative controls)and sexual behavior was monitored. PPT was as effective as E2 at maintaining mating behavior suggesting that, in the MPO, ERα is sufficient to mediate responses to E2 that underlie male rat mating behavior.

Estradiol

Sexual behavior

Dihydrotestosterone

Cholesterol

Estrogen receptor

propyl-pyrazole-triol (PPT)

Medial preoptic area

Actions of Selective Estrogenic Drugs Implanted Into the Medial Amygdala on Male Rat Mating Behavior

Dunigan, Anna I

04 April 2012

Estrogen stimulation of the medial amygdala (MEA) of the brain promotes male rat mating behavior. However, selective stimulation of either of the estrogen receptor subtypes found in the MEA (ERα or ERβ) does not support mating behavior. We tested the hypothesis that dual stimulation of ERα and ERβ is required to activate estrogen-dependant neural circuits in the MEA responsible for mating by local treatment of MEA with a combination of selective estrogenic agonists: propyl pyrazole triol (PPT, an ERα agonist ) and diarylpropionitrile (DPN, an ERβ agonist) administered to castrated, DHT maintained male rats. Estradiol (E2) or cholesterol (Chol) MEA implants served as positive and negative controls respectively. The animals receiving a mixture of PPT and DPN into the MEA displayed higher levels of mating behavior than the Chol treated animals but lower levels of mating behavior than the E2 treated animals.

Estradiol

Estrogen receptor

Medial amygdala

Sexual behavior

Propyl pyrazole triol (PPT)

Diarylpropionitrile (DPN)

Methyl-piperidino-pyrazole (MPP)

Mating