Session 11: Metabolic and Endocrine Control During Special Circumstances Flashcards
Metabolic fuels normally available in blood.
Glucose and fatty acids.
In which parts of the body can fatty acids not be used as fuel?
Red blood cells Retina of the eye Brain CNS
Metabolic fuels available under special conditions such as starvation.
Amino acids Ketone bodies Lactate
What hormones increase fuel concentrations?
Glucagon Adrenaline Growth hormone Cortisol
What hormones decrease fuel concentrations?
Insulin.
What is glucose stored as?
Glycogen.
What are fatty acids stored as?
TAGs
Where is glycogen stored? How much is stored?
In liver and muscles. Around 400g in total. Around 300g of it stored in muscles and approx. 100g of it stored in liver.
Acute effects of hypoglycaemia.
Trembling Weakness Tiredness Headache Sweating Sickness Tingling around lips Palpitations Changes in mood Slurred speech Stagerring walk
Effects of feeding.
Increased glucose uptake Storage of glucose as glycogen in liver and muscle Promotes amino acid uptake and protein synthesis in liver and muscle. Promotes lipogenesis and storage of fatty acids as TAGs in adipose tissue.
Effects of fasting.
Glycogenolysis Lipolysis Gluconeogenesis
Explain the key features of metabolic control from feeding to starvation.
Glucose and fat available from gut during the first few hours after feeding (2 hours ish) After 2 hours glucose and fats are no longer absorbed and the blood glucose necessary for the brain and red blood cells etc… is mainly drawn from glycogen stores. Other metabolic activity which are not dependent on blood glucose are maintained by fatty acids. At around 8-10 hours the glycogen storage deplete meaning that the brain needs to get its glucose elsewhere. This is now done by gluconeogenesis where the brain gets its glucose from amino acids, glycerol and lactate. Later on during starvation more proteolysis occurs but more importantly the brain starts to be able to utilise ketone bodies as a fuel which reduces the need for glucose.
Anabolic hormones.
Insulin and growth hormone where it increases protein synthesis.
Catabolic hormones.
Glucagon Adrenaline Cortisol Growth hormone where it increases lipolysis and gluconeogenesis (somewhat catabolic) Thyroid hormones
What processes stop the release of insulin.
Gluconeogenesis Glycogenolysis Lipolysis Ketogenesis Proteolysis
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Explain what happens in energy starvation.
What death is related with energy starvation?
Reduction of blood glucose stimulates release of cortisol from adrenal cortex and glucagon from pancreas.
Gluconeogenesis and breakdown of protein and fat occurs.
There is a reduction in the insulin to anti-insulin ratio which is due to cortisol. This prevent most cells from using glucose and fatty acids.
Glycerol from fat provides important substrate for gluconeogenesis reducing the need for breakdown of proteins.
Liver starts to produce ketone bodies. Brain uses glucose right now but will start use ketone bodies as well.
Kidneys begin to contribute to gluconeogenesis.
When the fat stores deplete protein will start to be used.
Death related to loss of muscle mass and resp. muscle infections.
Explain the fetal growth throughout pregnancy.
1/3rd of fetal growth occurs over the first 2/3rds of pregnancy.
2/3rds of fetal growth occurs over the last 1/3rd of pregnancy.
What are the two main phases of pregnancy?
Anabolic phase and catabolic phase.
Explain each phase of pregnancy.
Anabolic phase is early pregnancy where the mother increases their maternal fat stores* and there is a *small increase in level of insulin sensitivity. This is to prepare for rapid growth rate of foetus, birth and for subsequent lactation.
In late pregnancy catabolic phase will occur. There is now a decreased insulin sensitivity* and therefore an *increased insulin resistance.
Increase in insulin resistance results in an increase in maternal glucose and free fatty acid concentration.
Briefy explain placental transfer.
Most substances transfer by simple diffusion down concentration gradients.
Glucose is the principal fuel for foetus and transfer facilitaed by transporters which is mainly GLUT 1.
What is the fetoplacental unit?
The placenta, fetal adrenal glands and fetal liver of the foetus which forms a new endocrine entity to ensure the foetus own survival.
Explain the relationship between the placenta and the maternal hypothalamic pituitary axis.
The placenta secretes a wide range of proteins that can control the maternal hypothalamic pituitary axis and it does so mainly by influencing the release of corticotropin releasing hormone (CRH).
Oestriol and progesterone are two important placental steroid hormones as well.