Infertility-chapter from AT-Atariq
Holy Quran said
in
[the Night_stars
verses]
Now let
man but think from what he is created!"
6] He
is created from a drop emitted, ( seminal fluid )
[7]
Proceeding from between the backbone ( lumbar vertebral ) and the plives
anterior ( superior pubic-symphsis )
[8]
Surely (Allah) is able to bring semen back .
[9] The Day that
hypothalamus and anterior pituitary gland will be effected “
Scientists Link
Role of Insulin Receptors in Brain to Type 2 Diabetes, Appetite Control, Obesity
and Infertility
A new study led
by scientists at Joslin Diabetes Center and a German university links the
insulin signaling system in the brain not only to the onset of type 2 (adult
onset) diabetes, but also to appetite control, obesity and even infertility.
Using genetically-altered laboratory mice, the researchers found that the mice
in which insulin action was blocked gained weight at a considerably higher rate
than their counterparts, developed resistance to insulin action in other tissues
of the body, and exhibited a 50 percent decrease in fertility.
In a report
appearing in this week's journal Science, C. Ronald Kahn, M.D., and Deborah J.
Burks, Ph.D., of Joslin and their colleagues at the University of Cologne and
the European Molecular Biology Laboratory in Germany studied the effects of
"turning off" or deactivating insulin receptors in the brains of specially bred,
genetically-altered mice.
"We found
evidence of a decrease in the ability of insulin to lower blood glucose (sugar)
levels, increased appetite, obesity and increased infertility in the genetically
altered mice in which the insulin receptor in the brain had been genetically
knocked out," said Dr. Kahn, the Mary K. Iacocca Professor of Medicine at
Harvard Medical School.
Type 2
diabetes, which affects an estimated 16 million people in the U.S., often is
associated with obesity. In Type 2 diabetes, tissues of the body such as muscle,
liver and fat are resistant to the action of insulin, (known as insulin
resistance) while the pancreas produces some, but not enough, insulin, to
overcome this resistance. As a result, blood sugar (glucose) backs up in the
bloodstream. If poorly managed over time, elevated blood sugar levels can lead
to such complications as blindness, leg and foot amputations, kidney disease,
heart disease and stroke.
Scientists have
known for some time that insulin resistance and beta cell dysfunction in the
pancreas are the major contributors to Type 2 diabetes in people, but exactly
how insulin resistance might affect the brain has been unclear. Previous studies
have shown that insulin receptors and even insulin itself may be present in the
brain, and some work has demonstrated that insulin signaling in the brain may
contribute to eating behavior. Disruption of the insulin signaling system also
has been suggested to occur in such disorders as Alzheimer's and Parkinson's
disease.
Previous
studies have suggested a role for insulin signaling in the brain and
hypothalamus in the regulation of food "uptake" and body weight. Since insulin
acts as a growth factor in nerves in cultured cells, the research team wanted to
learn how brain development and well-being would be affected when insulin
receptors were deleted in the laboratory mice. This new study indicates that
insulin receptors and insulin signaling proteins throughout the central nervous
system play an integral role in regulating and metabolism, as well as appetite
and fertility.
"We created
Neural (brain)-Insulin Receptor Knock Out (NIRKO) mice with a neuron-specific
disruption of the insulin receptor gene," Dr. Kahn said. "Our data demonstrates
the central role of insulin resistance signaling in regulating energy disposal,
fuel metabolism and reproduction."
Although only
the female mice exhibited an increase in body weight on a normal chow diet, both
males and females exhibited obesity on a high fat diet. In addition, both male
and female mice had increased body fat by 1.5 to two-fold on the regular diet.
The females also ate 20 percent more food compared to the female controls. Blood
leptin levels (a measure of fat mass) were elevated 2.5 times in the females and
1.5 times in the male NIRKO mice. Leptin normally suppresses appetite, but this
effect was also apparently reduced in the NIRKO mice.
A very
surprising finding was the link between brain insulin signaling and
reproduction.
The NIRKO mice
exhibited reduced fertility due to defective regulation by the hypothalamus in
the brain of a hormone (luteinizing hormone) that impairs sperm production and
ovulation. The authors state that this may explain why some women with diabetes
and obesity experience menstrual disorders and even polycystic ovary disease.
The authors
concluded that when considered with previous studies, this study demonstrates
that genetically determined insulin resistance in classical insulin target
tissues, such as muscle and fat, may combine with insulin resistance in
non-classical target tissues, such as the brain and beta cell. This interaction
may occur synergistically, resulting in obesity, insulin resistance, glucose
intolerance, and high blood fat levels, leading to the complex metabolic
syndrome associated with type 2 diabetes.
MALE
REPRODUCTIVE PHYSIOLOGY
The
Hypothalamic-Pituitary-Gonadal Axis
The
hypothalamus is the integrative center of the reproductive axis and receives
messages from both the central nervous system and the testes to regulate the
production and secretion of gonadotropin releasing hormone (GnRH).
Neurotransmitters and neuropeptides have both inhibitory and stipulator
influence on the hypothalamus. The hypothalamus releases GnRH in a pulsatile
nature which appears to be essential for stimulating the production and release
of both luteinizing hormone (LH) and follicle stimulating hormone (FSH).
Interestingly and paradoxically, after the initial stimulation of these
gonadotropins, the exposure to constant GnRH results in inhibition of their
release. LH and FSH are produced in the anterior pituitary and are secreted
episodically in response to the pulsatile release of GnRH. LH and FSH both bind
to specific receptors on the Leydig cells and Sertoli cells within the testis.
Testosterone, the major secretory product of the testes, is a primary inhibitor
of LH secretion in males. Testosterone may be metabolized in peripheral tissue
to the potent androgen dihydrotestosterone or the potent estrogen estradiol.
These androgens and estrogens act independently to modulate LH secretion. The
mechanism of feedback control of FSH is regulated by a Sertoli cell product
called inhibin. Decreases in spermatogenesis are accompanied by decreased
production of inhibin and this reduction in negative feedback is associated with
reciprocal elevation of FSH levels. Isolated increased levels of FSH constitute
an important, sensitive marker of the state of the germinal epithelium.
Prolactin also
has a complex inter-relationship with the gonadotropins, LH and FSH. In males
with hyperprolactinemia, the prolactin tends to inhibit the production of GnRH.
Besides inhibiting LH secretion and testosterone production, elevated prolactin
levels may have a direct effect on the central nervous system. In individuals
with elevated prolactin levels who are given testosterone, libido and sexual
function do not return to normal as long as the prolactin levels are elevated.