Title: Mammalian sexual differentiation simple model
1Mammalian sexual differentiation (simple model)
Genetic Sex
Gonad (primary sex organ) Sex
Phenotypic Sex
- Key developmental neuroendocrine concept
- Organization versus activational effects of
hormones
2Male Female Sexual Development
- Lack of SRY results in formation of ovaries.
- No MIS allows Mullerian ducts to develop.
- No Testosterone results in Wolfian duct
regression. - Feminization and demasculinization Default or
Pre-Programmed Pathways
- SRY determines testis formation
- Sertoli cells in developing testis produce
Mullerian-inhibiting hormone (aka MIS). - Leydig cells in developing testis produce
testosterone. - MIS results in defeminization of accessory sex
organs. - Testosterone/DHT results in masculinization of
genitalia.
3Summary of Mechanisms Underlying Sexual
Dimorophisms in the Nervous System.
- Spinal nucleus of bulbocavernosous (SBN) produced
indirectly by masculinization of genitalia
(requires androgen receptor stimulation) during
perinatal development. - Sexually-dimorphic nucleus of the preoptic area
(SDN-POA) produced by estrogen-receptor
mediated reduction of apoptosis during perinatal
development. - Medial amygdala posterior dorsal (MeApd)
produce by estrogen-receptor stimulation that
must be maintained throughout life.
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5Classifications of Behaviors
- Consummatory behavior behaviors exhibited
during completion of a motivated behavior.
Consummatory sexual behaviors copulation. - Appetitive behavior all behaviors an organism
exhibits when attempting to gain access to a
positive reinforcer (or avoiding a negative
reinforcer). Appetitive sexual behaviors
behaviors exhibited in order to gain access to an
sexual partner.
Appetitive behaviors facilitate or arouse
consummatory behaviors
Temporal-Relational Model
Appetitive behavior
Consummatory behavior
Consummatory behaviors tend to diminish
appetitive behaviors
6The Hypothalamus-Pituitary-Gonadal Axis
- The brain is the overall controller of
circulating gonadal steriods. - Gonatopropin Releasing Hormone (GnRH) release by
hypothalamus to stimulate anterior pituitary. - Gonadotroph cells in anterior pituitary release
Luteinizing hormone (LH) follicle stimulatin
hormoner (FSH). - LH stimulates Leydig cells in testis to release
testosterone. - FSH stimulates sertoli cells to produce sperm.
- Testosterone feedbacks to influence brain
function, particularly those relating to
reproduction.
7Hormonal Control of Male Sexual Behavior Summary
- Sexual behavior in both rodent and primate males
is regulated by steriod hormones. - Males have relatively constant levels of steroids
and behavior. - Both male sexual behavior is influenced by both
androgen receptor (erection) and estrogen
receptor (brain) stimulation.
8mPOA, DA, T in Male Copulation
- Glutamate is increased by sexual stimulation.
- Glutamate stimulates NMDA receptors which
activates NOS. - Increased NO stimulates DA release and/or reduces
reuptake.
mPOA serves complex role in regulating sexual
behavior -integration of environmental stimuli
genital stimulation to trigger arousal/excitement
ejaculaiton.
- Roles of DA receptors in the mPOA during
copulation. - low threshold D2R respond to sensory stimuli
(e.g. chemosensory) to facilitate erection. - D1R respond to senory and genital (copulation)
stimulation to maintain erection. - High threshold D2R initiate ejaculation.
ER stimulation increases NOS making mPOA more
responsive to glutamate during sexual
stimulation-gt-gtinc DA release
Glutamate comes from MEA (chemosensory)
brainstem (genital)
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10Endocrine Function in Rat Estrus Cycle
Diestus Low E P, releases LH FSH from
negative feedback and LH FSH rise producing
growth of follicle which increases E. Proestrus
Hypothalamic GnRH control of LH FSH regulated
by E in positive feedback (unknown mechanism)
resulting in LH surge that causes ovulation.
Estrus Hypothalmus returns to negative feedback
by E P. Corpus luteum grows giving rise to
increases in progresterone.
Notes Estrous (behavior) proestrus (endocrine)
phase Similar (perhaps identical) hormonal
regulation in menstrual and estrus cycles
11The Ovary during Menstrual Cycle
P
FSH
LH Surge
Graffian Follicle
E
- Under control of LH FSH, a follicle develops
and is released at ovulation LH FSH are
peptides that bind to cell-suface receptors on
granulosa and theca cells and activate
steroidogenic enzymes. - Follicular Phase FSH induces follicular to grow
and estrogen is produced by granulosa cells of
the follicle as follicle grows more E is
released. - Periovulatory Period LH surge causes Graffian
Follicle to rupture releasing ova. LH surge
produced by E acting to stimulate HPG (positive
feedback) - Luteal Phase Progesterone is produced by Corpus
luteum.
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13Estrous versus Menustral Cycle
14Neural Control of Sexual Behavior
MPOA and VMH mutually inhibit each other to
control dynamics of lordosis and active
components of female sexual behavior.
MPOA
15The Sexual Brain
NAc
LH
VTA
- The medial preoptic area (MPOA) is critical for
(active) copulatory behavior it receives direct
and indirect input from brain areas that are
important for the assimilation of sexually
relevant information. - Pheromonal stimulation is received by the
olfactory bulbs (OB), the OB project to the
medial amygdala (MeA), which relays information
to the bed nucleus of stria terminalis (BST) and
the MPOA. - Additionally, the MPOA and MeA receive
somatosensory input (from genitals) via the
central tegmental field (CTF). - In turn, the MPOA projects to the ventral
tegmental area (VTA) and the brain stem (BS)
which project to cortico-limbic structures. - Nucleus accumbens (NAc), basolateral amygdala,
and cortical structures are critical for
motivational processes particularly for
sexually-conditioned stimuli. - Lateral hypothalamus involved in inhibiting mPOA
and NAc.
16Types of Information Storage aka Learning/Memory
- Info storage system(s) in the brain acquires,
stores (consolidation), and retrieves information
to organize future behavior. - There are multiple types of memory which seem to
have somewhat independent neural substrates.
(Learning)
17Stress Memory
Acute mild to moderate stress (i.e. not
traumatic) has a bi-modal influence of the
storage of information.
- Epinephrine bimodally influence consildation
(post-event encoding of information). - Epi -gt Glucose -gt insulin -gt brain(?)
- -gt peripheral Rec - gt feedback to brain (?)
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19Sex differences in human brain
- There are sex differences in neurotransmitter
levels between men and women - 5HT lower in women
- DA higher in women
- Also regionalization of neuropeptides e.g.
vasopressin. - Differences in receptor expression are also
reported and important for transmission.
- Male brain gt female brain.
- These differences are corrected for overall size
20Sex Difference in Neurotransmitters
- There are sex differences in neurotransmitter
levels between men and women - 5HT lower in women
- DA higher in women
- Also regionalization of neuropeptides e.g.
vasopressin. - Differences in receptor expression are also
reported and important for transmission.
Nishizawa and colleagues used positron emission
tomography (PET) to assess serotonin synthesis
rates in healthy men and women. a Images show
PET scans taken from a representative male and
female subject. Images are shown before and after
depletion of plasma tryptophan. The mean rate of
synthesis was found to be 52 higher in males
than in females. b Magnetic resonance images
for reference taken from the same level as the
PET images. The results may help to explain why
some disorders (such as unipolar depression) that
involve serotonin dysfunction do not equally
affect men and women.
21Sex Difference Cognition
- Sex difference have been recognized in a variety
of behaviors, including cognition, reflect
combined organizational and activational effects
of steroids and experience on the nervous system. - Organizing effects occur perinatally, puberty,
and adult (e.g. chronic stress later)
22Sex Difference in Stress Cognition
- ACUTE STRESS
- Males and females show opposite effects to acute
stress. - Acute stress increases male dendritic trees but
decrease those of females. - Males also perform better on stress related
learning (e.g. larger improvements in
consolidation effects). - CHRONIC STRESS
- affects male hippocampus much more than females
(not affected by typical 2-3 week protocols). - Effects on spatial memory match these
morphological changes. - Only limited stress paradigms have been examined
(i.e. could be increased resistance not
immunity).
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