Demasculinization of male Japanese quail by prenatal estrogen treatment

Genetic male Japanese quail were administered sex hormones or the oil vehicle on Day 10 of incubation and were caponized 3 weeks after hatching. As adults, the capons were injected with testosterone propionate daily for 2 weeks and then were tested for masculine sexual behavior in response to sexually receptive females. Males that had received as little as 2 μg of estradiol-17β in ovo failed to exhibit the head grabbing and mounting typical of the normal masculine sexual response to females. In a second experiment, this demasculinization was produced by prenatal treatment with 2 μg of estradiol-17α, estrone, estriol, or diethylstilbestrol, but not by this quantity of testosterone. These data suggest that an estrogen is the agent of behavioral demasculinization in the normal female, and that endogenous testosterone poses no difficulty for proper sexual development in the normal male.     

Specific activation of estrogen receptor alpha and beta enhances male sexual behavior and neuroplasticity in male Japanese quail

Two subtypes of estrogen receptors (ER), ERα and ERβ, have been identified in humans and numerous vertebrates, including the Japanese quail. We investigated in this species the specific role(s) of each receptor in the activation of male sexual behavior and the underlying estrogen-dependent neural plasticity. Castrated male Japanese quail received empty (CX) or testosterone-filled (T) implants or were daily injected with the ER general agonist diethylstilbestrol (DES), the ERα-specific agonist PPT, the ERβ-specific agonist DPN or the vehicle, propylene glycol. Three days after receiving the first treatment, subjects were alternatively tested for appetitive (rhythmic cloacal sphincter movements, RCSM) and consummatory aspects (copulatory behavior) of male sexual behavior. 24 hours after the last behavioral testing, brains were collected and analyzed for aromatase expression and vasotocinergic innervation in the medial preoptic nucleus. The expression of RCSM was activated by T and to a lesser extent by DES and PPT but not by the ERβagonist DPN. In parallel, T fully restored the complete sequence of copulation, DES was partially active and the specific activation of ERα or ERβ only resulted in a very low frequency of mount attempts in few subjects. T increased the volume of the medial preoptic nucleus as measured by the dense cluster of aromatase-immunoreactive cells and the density of the vasotocinergic innervation within this nucleus. DES had only a weak action on vasotocinergic fibers and the two specific ER agonists did not affect these neural responses. Simultaneous activation of both receptors or treatments with higher doses may be required to fully activate sexual behavior and the associated neurochemical events.     

Age-related reproductive decline in the male Japanese quail

A series of experiments was conducted to study the decline in reproduction associated with age in the male Japanese quail. In Experiment 1, eggs were collected from pairs that were 28, 56, 107, and 149 weeks of age. Pairs that were 56 weeks of age or older showed a sharp drop in fertility and hatchability. Subsequent experiments were designed to study the endocrine and behavioral basis for this decline in the male. In Experiment 2, males that were between 23 and 70 weeks of age were tested for mating behavior, plasma testosterone was measured, and testes wet weight was determined. There were no significant differences between the age groups. However, samples taken from an additional group of males 168 weeks of age showed significantly (P < 0.05) lower serum testosterone and testes weight. Therefore, the third experiment was designed to include age groups of males between 4 and 126 weeks of age in order to further examine this decline in males older than 70 weeks of age. There was a significant (P < 0.05) drop in this number of males showing sexual behavior and of those males showing sexual behavior; the quantity of mating activity also declined. Plasma testosterone was reduced in the older groups; however, the change was not significant. In addition, the size of the cloacal gland, an androgen-dependent organ, declined with age (P < 0.05). These results argue that the age-related reproductive decline may have behavioral as well as endocrine basis. Possibly, the behavioral changes may result from altered receptor sensitivity at the level of areas of the brain, which control reproductive behavior, and at the level of the testes, which affect hormone production and spermatogenesis.     

Antifertility effect of gossypol in male Japanese quail

Conventionally housed 130-160 g adult male Japanese quail were given gossypol acetic acid (gossypol) im at 25 mg/kg in 0.5 ml of 10% EtOH for 12 and 24 days (Groups 1 and 2), respectively. One day after treatment was terminated they were allowed to mate with laying females individually for 20 days. Fertility was 0% from mating of the Group 1 birds on days 1-2 and increased to 25, 35, 55 and 65% on days 3-6 after cessation of gossypol treatment. At day 11, fertility was 80 vs 84% in controls, whereas hatchability was 70% for both. By comparison, eggs from Group 2 mated quail were infertile for up to 20 days after the termination of gossypol treatment. In a parallel experiment, the percent testes to body weight ratio in control and 7, 14, 21, and 28-day gossypol-treated quail was 2.5, 2.2, 1.8, 0.5, and 0.2%, respectively. In 12 vs 24-day treated birds, 7, 14, 21, and 28 days after gossypol treatment, the ratios were 1.0 vs 0.5%, 2.0 vs 0.8% and 2.8 vs 1.9%, respectively. The decreased fertility and hatachability, and testicular atrophy resulting from gossypol given to male quail was dose-time related. Furthermore, the androgen-dependent cloacal gland was drastically reduced in size by the treatment with gossypol. The mode of action of gossypol in male quail is different than it is in mammals in that the testicular size of mammals remains unchanged with long-term gossypol treatment. It is concluded that quail may be a useful avian animal model for investigating the antifertility effects of gossypol.     

Cocaine-induced sensitization correlates with testosterone in male Japanese quail but not with estradiol in female Japanese quail

Research has indicated that gonadal hormones may mediate behavioral and biological responses to cocaine. Estrogen, in particular, has been shown to increase behavioral responding to cocaine in female rats relative to male rats. The current study investigated the effect of cocaine on locomotor activity and hormonal correlates in male and female Japanese quail (Coturnix japonica). In Japanese quail, circulating hormone levels can be manipulated without surgical alterations via modifying the photoperiod. Male and female quail were housed on either 8L:16D (light:dark) or 16L:8D (light:dark) cycle for 21 days. Blood samples were taken prior to the beginning of the experiment and assays were performed to determine the levels of testosterone (T) and estradiol (E2). Quail were given injections of saline or cocaine (10 or 20 mg/kg) once a day for 10 days. Immediately after each injection, birds were placed in open field arenas and distance traveled was measured for 30 min. Results showed that male quail housed under long-light conditions exhibited cocaine-induced sensitization to 10 mg/kg cocaine which was correlated with the high levels of plasma T. Female quail housed under short-light conditions demonstrated sensitization to 10 mg/kg cocaine, but this was not correlated with the levels of plasma E2. The current findings suggest that cocaine-induced locomotor activity was associated with T in males but not with E2 in females.     

Differential bone and muscle recovery following hindlimb unloading in skeletally mature male rats

This study was designed to track the recovery of bone and muscle properties after 28 days of hindlimb unloading (HU) in skeletally mature male rats in order to quantify the degree and timing of the expected mismatch between bone and muscle properties. Outcome variables were in vivo plantarflexor peak isometric torque and proximal tibial volumetric bone mineral density (vBMD). Proximal tibia vBMD was significantly lower than age-matched controls (-7.8%) after 28 days of HU, continued to decrease through day 28 of recovery (-10%) and did not recover until day 84 of recovery. Plantarflexor peak isometric torque was significantly reduced after 28 days of HU (-13.9%). Further reductions of isometric torque occurred after 7 days of recovery (-15%), but returned to age-matched control levels by day 14. The functional relationship between bone and muscle (vBMD/isometric torque) tended to increase after 28 days of HU (+7.8%), remained elevated after 7 days of reloading (+9.1%) and was significantly lower than age-matched controls on day 28 (-13.6%). This relatively rapid return of muscle strength, coupled with continued depression of bone density at the proximal tibia metaphysis, may increase the risk for skeletal injury during recovery from prolonged periods of reduced mechanical loading.     

Increased bone mass in male and female mice following tamoxifen administration

Tamoxifen is capable of preserving bone mass in gonadectomized rodents as well as intact female mice; however, a detailed 3D quantitative analysis of the structural changes produced in the growing skeleton of intact mice of both genders by this agent is lacking. Employing quantitative microcomputed tomography (muCT), we assessed the effects of 4-hydroxytamoxifen (OHT) on the femora of C57BL/6J mice administered this agent either for 12 (males and females) or 2 (females) weeks. In mice of either gender, but especially in females, 12 weeks of OHT exposure led to dramatic increases in both cortical and trabecular bone. Females exposed to OHT for either 2 or 12 weeks demonstrated significantly increased cortical wall thickness, trabecular bone volume, connectivity, and number, as well as decreased trabecular separation. Significant increases in several of these parameters were also evident in males after 12 weeks of OHT administration. In view of the expanding use of OHT to induce Cre-mediated recombination events, our findings suggest that care should be exercised when interpreting the skeletal phenotypes of mice exposed this agent, particularly in situations where the effects of OHT might synergize with the phenotypic outcome of a specific genetic alteration.     

Sexual experience modulates neuronal activity in male Japanese quail

After an initial increase, repeated exposure to a particular stimulus or familiarity with an event results in lower immediate early gene expression levels in relevant brain structures. We predicted that similar effects would occur in Japanese quail after repeated sexual experience within brain areas involved in sexual behavior, namely, the medial preoptic nucleus (POM), the bed nucleus of stria terminalis (BST), and the nucleus taeniae of the amygdala (TnA), an avian homolog of medial amygdala. High experience subjects copulated with a female once on each of 16 consecutive days, whereas low experience subjects were allowed to copulate either once or twice. Control subjects were never exposed to a female. High experience subjects were faster to initiate sexual interaction, performed more cloacal contacts, and completed each cloacal contact faster than low experience subjects. Low experience subjects showed an increase in egr-1 (ZENK) expression, an immediate early gene product used as marker of neural activation in birds, in the areas of interest. In contrast, in high experience animals, egr-1 expression in the POM, BST, and the periaqueductal gray (PAG) was not different than the level of expression in unmated controls. These results show that experience modulates the level of immediate early gene expression in the case of sexual behavior. Our results also indicate that immediate early gene expression in specific brain areas is not necessarily related to behavioral output but depends on the behavioral history of the subjects.     

Effects of cyproterone acetate in the male Japanese quail

Male Japanese Quail were injected with oil or with one of four dosages of cyproterone acetate for 8 days. Copulatory behavior and cloacal gland size were measured daily. Cyproterone acetate reduced cloacal gland size at all dosages and in two experiments reduced copulation in eight out of 17 males at the two highest dosages. Thus, cyproterone acetate results in reproductive changes in at least two classes of vertebrates, and has behavioral as well as morphological effects. The morphological effects are more striking, however.     

Chronic pre-exposure to methamphetamine following 31 days of withdrawal impairs sexual performance but not sexual conditioning in male Japanese quail

In the current study, male quail were administered methamphetamine (3.0 or 5.6mg/kg IP) or saline once daily for 10 days and locomotor activity was assessed. Following a 31-day withdrawal period, sexual conditioning trials were conducted such that a conditioned stimulus (CS) was presented prior to a copulatory opportunity with a female quail. Male quail treated with methamphetamine (5.6mg/kg) showed a decrease in locomotor activity from Trial 1 to Trial 10 suggesting a potential tolerance effect. Following the 31-day withdrawal period, all male quail that received the CS paired with a copulatory opportunity showed enhanced approach to the CS, regardless of treatment history. Thus, chronic pre-exposure to methamphetamine did not alter sexual conditioning. In contrast, chronic pre-exposure to methamphetamine (3.0mg/kg) decreased the frequency of successful copulations suggesting that it impaired sexual performance. The findings suggest that methamphetamine may differentially affect the neural circuitry involved in motivational systems compared with those involved in consummatory aspects of sexual behavior. These effects may last long after drug cessation.     

Agonistic behaviour and endogenous plasma hormones in male Japanese quail

Agonistic relationships established among male Japanese quail (Coturnix coturnix) in shortterm dyadic encounters of a round-robin tournament were stable and appeared to be maintained by a form of recognition. The aggressive or submissive behaviour displayed by competitors throughout the tournament did not relate to their circulating levels of luteinizing hormone, androstenedione, 5 α-dihydrotestosterone or corticosterone. However, plasma levels of testosterone were correlated with fighting success in the early phases of the tournament, before agonistic associations were defined. Once relationships stabilized, levels of plasma testosterone in winners declined to values comparable with those of the losers and the qualitatively distinct displays observed in winners or losers were no longer correlated with plasma levels of testosterone. In light of other work, these data suggest that androgens, primarily testosterone, influence the aggressiveness of an individual in initial encounters, helping in turn to determine dominance relationships between opponents. Thereafter, other factors such as learned response biases take precedence. The maintenance of stable social relationships appears to be independent of circulating levels of testosterone in adult male Japanese quail.     

The glycosaminoglycans of estrogen-induced medullary bone in Japanese quail

Glycosaminoglycans were isolated from the femurs of estrogen-treated male Japanese quail. During the 72 h after the injection of estrogen the incorporation of a 1-h pulse of H₂³⁵SO₄ into keratan sulfate increased more than 100-fold in a pattern corresponding to the production of the induced medullary bone. The rate of incorporation into chondroitin 4-sulfate, the only other glycosaminoglycan detected, remained constant throughout the same time period. The rate of incorporation of the 1-h pulse of sulfate into chondroitin 4-sulfate and keratan sulfate was the same at 48 h of estrogen treatment. When birds (48 h estrogen) were allowed to live 6 h after the injection of the isotope, chondroitin 4-sulfate accumulated 5-fold over that found for similar animals labeled for only 1 h. Keratan sulfate, into which the isotope was incorporated at the same rate as the chondroitin sulfate in this experiment, did not accumulate much more in 6 h of labeling than in 1 h of labeling. This suggests that the keratan sulfate turns over more rapidly than the chondroitin 4-sulfate in this tissue. Autoradiography showed that the chondroitin 4-sulfate was associated mainly with the marrow cells near the cortical bone and the keratan sulfate with the newly synthesized medullary bone. These results suggest that keratan sulfate is a specific marker for this secondary bone matrix.     

Immunoelectron microscopic demonstration of estrogen receptors in osteogenic cells of Japanese quail

The localization of estrogen receptors (ERs) in osteogenic cells was immunoelectron microscopically examined in the femurs of female and estrogen-treated male Japanese quail. An electron dense reaction product showing ER localization was observed in the nuclei of osteoblasts and immature osteocytes in the medullary bone of the female quail. However, reaction product was not seen in the osteoclasts. On the endosteal bone surface of male quail, nuclear reaction product was detected in bone lining cells. After 24 h of estrogen treatment, reaction product was observed in the nuclei of preosteoblasts on the endosteal bone surface. After 48 h, the medullary bone partly appeared along the endosteal surface. Nuclear reaction product was seen in osteoblasts on the medullary bone surface.     

Immunoelectron microscopic demonstration of estrogen receptors in osteogenic cells of Japanese quail

Summary The localization of estrogen receptors (ERs) in osteogenic cells was immunoelectron microscopically examined in the femurs of female and estrogen-treated male Japanese quail. An electron dense reaction product showing ER localization was observed in the nuclei of osteoblasts and immature osteocytes in the medullary bone of the female quail. However, reaction product was not seen in the osteoclasts. On the endosteal bone surface of male quail, nuclear reaction product was detected in bone lining cells. After 24 h of estrogen treatment, reaction product was observed in the nuclei of preosteoblasts on the endosteal bone surface. After 48 h, the medullary bone partly appeared along the endosteal surface. Nuclear reaction product was seen in osteoblasts on the medullary bone surface.     

Effects of triiodothyronine and estrogen administration on bone mass, mineral content and bone strength in male rats.

Experimental hyperthyroidism had a negative effect on bone mineral density, but did not significantly alter mechanical properties of femur and femoral bone thickness. Estradiol at a dose used in humans for the treatment of osteoporosis decreased seminal vesicle weight and concentration of testosterone but increased bone density in male rats compared to intact animals. In these rats, the mechanical analysis revealed an increased mechanical femur strength higher than the increase in bone density and femoral cortical thickness. When hyperthyroid male rats with low bone density were treated with estradiol in spite of a low plasma testosterone, the changes in bone density resulting from hyperthyroidism were entirely prevented. Estrogens protect the male skeleton against resorbing action of T (3). Treatment with estradiol in male rats with hyperthyroidism did not increase mechanical bone strength or femoral cortical thickness as it did with estradiol administration alone. Our results suggest that exogenously administered estrogens may have therapeutic value in preventing bone loss accompanying triiodothyronine administration, even in male rats with a low testosterone levels. At the concentration studied, estradiol increased in spite of low plasma testosterone, bone mineral density, mechanical strength of femur, and femoral cortical thickness.     

Daily patterns of courtship and mating behavior in the male Japanese quail

Crowing behavior was monitored constantly in male Japanese quail housed singly over 30 successive days. The photoperiod was 16h of light and 8 h of dark. A daily pattern in crowing was observed in which the frequencies were elevated in the afternoon and at the beginning of darkness. However, peak crowing occured 2 h prior to the onset of light. These rhythms were highly correlated among individuals and extremely repeatable over the sequential days of observation.In a second experiment, males which were paired with females were observed for frequencies of crowing, courtship, and mating behavior during the lighted portion of the day. In this experiment, the same photoperiod (16L:8D) was maintained. Paired males exhibited a daily pattern in crowing similar to that observed in the singly housed males. The frequency of mating was the highest between 1200 and 1300 h and lowest at 1400 h. Mating success was highest at midday, as were the number of males exhibiting mating behavior. These diurnal patterns in sexual behavior may depend on environmental cues such as photoperiod, which, in turn, may stimulate endocrine triggers.     

Rapid effects of aromatase inhibition on male reproductive behaviors in Japanese quail

Non-genomic effects of steroid hormones on cell physiology have been reported in the brain. However, relatively little is known about the behavioral significance of these actions. Male sexual behavior is activated by testosterone partly through its conversion to estradiol via the enzyme aromatase in the preoptic area (POA). Brain aromatase activity (AA) changes rapidly which might in turn be important for the rapid regulation of behavior. Here, acute effects of Vorozole, an aromatase inhibitor, injected IP at different doses and times before testing (between 15 and 60 min), were assessed on male sexual behavior in quail. To limit the risk of committing both types of statistical errors (I and II), data of all experiments were entered into a meta-analysis. Vorozole significantly inhibited mount attempts (P < 0.05, size effect [g] = 0.527) and increased the latency to first copulation (P < 0.05, g = 0.251). The treatment had no effect on the other measures of copulatory behavior. Vorozole also inhibited appetitive sexual behavior measured by the social proximity response (P < 0.05, g = 0.534) or rhythmic cloacal sphincter movements (P < 0.001, g = 0.408). Behavioral inhibitions always reached a maximum at 30 min. Another aromatase inhibitor, androstatrienedione, induced a similar rapid inhibition of sphincter movements. Radioenzyme assays demonstrated that within 30 min Vorozole had reached the POA and completely blocked AA measured in homogenates. When added to the extracellular milieu, Vorozole also blocked within 5 min the AA in POA explants maintained in vitro. Together, these data demonstrate that aromatase inhibition rapidly decreases both consummatory and appetitive aspects of male sexual behavior.