The volume of SDN in medial preoptic area is modified by hormones, among which testosterone is proved to be of much importance. The larger volume of male SDN is correlated to the higher concentration of fetal testosterone level in males than in females. Also, there is evidence that testosterone acts during specific prenatal period to organize the development of aromatase-expressing neurons into the male-typical SDN (testosterone is transformed to estrogen by aromatase). The effect of testosterone is also reflected by the influence of fetal intrauterine position on the morphology of SDN-POA. Studies demonstrated that male rats which were gestated between two male fetuses (2M) have 2-fold larger SDN-POA volumes than those gestated between two female fetuses (2F). At the same time, the testosterone levels, as well as the 17β-estradiol (product of testosterone) levels, were found to be significantly larger in 2M males than in 2F males on gestation day 21 (testosterone can be transferred from adjacent male fetuses to the target rats). However, evidence fails to show any relationship between SDN volume and female fetal position.
According to some studies, the volume difference of SDN between males and females is related to apoptosis during early development after birth. In rats, central division of the medial preoptic nucleus (MPNc) is an important component of SDN-POA and evidence showed that the number of apoptotic cells within MPNc is greater in females than in males between postnatal day (PD) 7 and PD10. In MPNc, the levels of some proteins, which are related to apoptosis, were shown to be of significant difference between males and females. Such proteins include Bcl-2 and Bax. Bcl-2 is an antiapoptotic protein. The level of Bcl-2 in PD8 male rats is much higher than that in female rats of the same age, hence the number of apoptotic cells of MPNc in PD8 male rats is much lower than PD8 female rats. On the other hand, Bax, a proapoptotic protein, shows lower level in PD8 males than in PD8 females. Also, the number of active caspase-3-ir cells was observed to be greater in females than in males, indicating higher level of apoptosis in female MPNc.
Apoptosis also occurs in the anteroventral periventricular nucleus (AVPV), which is also a sexually dimorphic area and is located in the periventricular gray area at the rostral extreme of the third ventricle. In contrast with SDN-POA, AVPV has larger size in females than in males. It is proved that Bcl-2 level in AVPV is higher whereas Bax level is lower in females than in males, just as being opposite of those in MPNc. As indicated in these two cases, apoptotic cell death plays a critical role in the formation of sexually dimorphic nucleus, and the apoptotic cell number within SDN negatively correlates with the volume of SDN between different sexes.
Male sexual behaviors can be divided into two phases: the appetitive phase, which contains highly variable sequence of behaviors such as attracting and courting, and the consummatory phase, during which highly stereotyped copulatory behaviors occur. The medial preoptic area of the brain is considered to control the expression of both male copulation and male appetitive sexual behavior. It is found that large lesions of SDN-POA severely disrupt copulatory behavior in rats. Also, cell-body lesions of SDA pars compacta (a homology of SDN-POA) in gerbils produce severe disruptions of male copulatory behavior. Moreover, a study on medial preoptic nucleus (POM) (homologue of medial preoptic nucleus in rats) in quails showed that the activation of male copulatory behavior requires the aromaticity of androgen (testosterone) into an estrogen (17β-estradiol). Like in SDN-POA, aromatase-expression neurons are a specific marker of the nuclear boundary of POM in squails. The intensity of male copulatory behavior is found to positively correlate with the number of the aromatase-expression neurons in the caudal part of POM.
Appetitive behaviors are also partly controlled by medial preoptic area as aromatase-knockout mice show deficits in sexual motivation. However, appetitive behaviors are disrupted by the lesions in rostral part rather than caudal part of medial preoptic area. Lesions of the rostral part of medial preoptic area also diminish preference for female by male rats. Furthermore, in vivo dialysis experiments showed that the level of extracellular dopamine in the mPOA increases as the sexual appetitive sequences progress. mPOA’s involvement in the control of appetitive sexual behaviors is also confirmed by pharmacological manipulations of the dopaminergic system in it. In rats, lesions to mPOA can eliminate the male copulatory behavior but can only diminish appetitive behavior, which suggests that some other parts of the brain, except for mPOA, are also responsible for sexually appetitive behavior.
Other species have similar relationships between sexual preferences and the volume of SDN. For example, INAH3 in humans (homologue of oSDN) is significantly larger in heterosexual men than in homosexual men.
Bilateral damage to SDN in the medial preoptic area in male ferrets causes the change of males from male-typical preference to female-typical preference. Male ferrets which were sexually experienced and responded to female body odor, when treated by bilateral lesions to SDN, change to respond to male body odor. It is probable that SDN plays an important role in leading to mating and successful reproduction.
Although SDN is much related to sexual partner preferences in males, it does not show the same relationship to partner preferences in females. Evidence shows that SDN in medial preoptic area is not the prerequisite for the expression of male-typical sexual behaviour and sexual partner preferences in females. One piece of evidence comes from the study on female Japanese macaque, which routinely court, mount (with pelvic thrust), compete for, and even prefer certain female sexual partners over certain males. The part of the brain examined is the anterior hypothalamic nucleus (AHdc), a homologue of SDN-POA. Comparison of the AHdc nucleus volumes between Japanese macaque and rhesus macaque (a closely related sister species of Japanese macaque) shows that there is no significant difference between the volume of AHdc in more male-typical macaques and that in female-typical macaques.
NELL2 is a tissue-specific protein in the nervous system. It contains EGF (epidermal growth factor)-like repeat domain and its gene expression is regulated by estrogen. NELL2 is also known to play a neuroprotective role rat hippocampus neurons. When NELL2 synthesis is blocked by intracerebroventricular injection of antisense (AS) NELL2 oligodeoxynucleotide (ODN) into neonatal male rat brains (postnatal day0-day5), the size of SDN-POA is decreased. Since volume of SDN is related to the level of testosterone, it is quite possible that the volume is finally due to the neuroprotective effect of estradiol which is produced from testosterone by aromatase. So the result that NELL2 blockage reduces the size of SDN-POA suggests that it probably has neuroprotective effect on SDN-POA.
The sex-specific transcription of somatostatin gene coincides with the establishment of sex differences in SDN-POA. It is observed that somatostatin mRNA appears in the SDN-POA of both males and females. On postnatal day 8 through postnatal day 35, the area of somatostatin mRNA-positive cells was significantly larger in males than in females, with males attain the maximum size of that area on day15 before decrease whereas females show no changes. Eventually the expression of somatostatin mRNA shows no difference between sexes. It is possible that somatostatin is related to the estrogen-dependent organization of SDN-POA.
Fenitrothion is a kind of organophosphate and it can affect the development of reproductive system of male rats. Treatment with fenitrothion to male rats causes regression of androgen-dependent organ weights because fenitrothion is a potent competitive androgen receptor antagonist. Its effect on SDN-POA is different between male rats and female rats. In male rats, prenatal exposure to fenitrothion causes significantly increase of the volume of SDN-POA; whereas, in female rats, prenatal exposure to fenitrothion causes significantly decrease of the volume of SDN-POA. One possible explanation is that fenitrothion can alter the activity of aromatase, which then alters the level of estrogens converted by it from androgens and finally alters the volume of SDN-POA.
Diethylstilbestrol (DES) is a synthetic nonsteroidal estrogen and was widely used for preventing threatened abortion. DES also has effect on development of the reproductive system. Low dose of DES exhibits inhibitory effect on plasma testosterone concentration in male rats while promotes follicular maturation in female rats. Experiments were done to see the effects of DES on SDN-POA volume. It is demonstrated that DES treatment altered the volume of SDN-POA in females by increasing it, resulting in larger volume SDN than controlled females. However, low dose of DES did not change the volume of SDN-POA in male rats.
Morphine can also alter the activities within the sexually dimorphic brain regions. Prenatal exposure to morphine increases copulatory behavior in male rats while decreases estrous behavior in female rats.
Ventromedial nucleus of the hypothalamus (VMN) has long been considered as a sexually dimorphic nucleus. It is an important region for regulating the sexual responses in female rodents. The neurons within VMN have significant estrogen-dependent functional and structural plasticity. The synaptic organization of the VMN is sexually dimorphic. Females have more dendrite chemical synapses within VMN while males have more somatic synapses within that region. In addition, the size of postsynaptic densities of axospinous and axosomatic synapses is sexually dimorphic, with males having larger density than females. Estrogen plays an important role in modulating the sexually dimorphic synaptic connectivity of VMN. Estradiol levels are high on proestrus rats and return to low levels on diestrus rats. The volume of cell bodies within VMN in estrous cycle rats and male rats is larger than estrous cycle rats. Also, proestrus rats have significantly higher synapse density in VMN than diestrus rats. Moreover, Gamma-aminobutyric acidplays a role in VMN development such as sexual differentiation.