OS - Appetite/Satiety Regulation
Leptin
(an anorexigenic hormone) wants to inhibit eating & appetite - orexigenic pathways are inhibited by its increase or stimulated by its decrease
PVN (paraventricular nucleus)
-Regulates both the anabolic and catabolic activities of adiposity via the ANS. -Stimulates sympathetic or parasympathetic systems depending on need -its neurons project to the medullary DMV and spinal intermediolateral column
GLP-1 (glucagon-like peptide)
-Released from ileum & colon -Elicited (most likely) by reflex activity from stomach & duodenum (gastro- intestino--ccoolliicc reflex?) -Acts on anorexigenic hypothalamic pathways to ---stimulate insulin release (parasympathetic) ---inhibit glucagon release, GI motility, and secretion ("ileal brake") -Acts on amygdala (in limbic system to generate malaise
PYY (peptide YY)
-Released from ileum/colon -Reduces GI motility (ileal brake) -Released by gastric food intake (reflex?) and fat in ileum -Stimulates hypothalamic anorexigenic pathways
insulin
-Released from pancreas -Short term responses: released from β-cceellllss in response to glucose levels -Long term responses released from β-cceellllss in response to FFA stemming from visceral fat -Insulin levels proportional to amount of visceral fat ---visceral fat leads to insulin resistance ---increased glucose releases more insulin
leptin
-Released from sub Q fat proportional to amount of sub Q fat present -Even in cases with high visceral fat, there is substantial abdominal subQ fat
neural route (peripheral signals)
-Vagal nerrve mediates physical and hormonal signals to solitary nucleus (NTS) in medulla -NTS projects to both hypothalamus and limbic system
leptin and insulin
-signal adiposity and elicity satiety -act on hypothalamic nuclei to suppress appetite and regulate fat storage
lower GI satiety signals
1. GLP-1 (glucagon-like peptide) 2. PYY - peptide YY
Model for regulation of the brain stem response to satiety signals by hormonal input from the ARC
Adiposity signals, insulin and leptin, signal body fat mass and stimulate hypothalamic ARC neuronal projections to LH & PVN. LH and PVN neurons project to the NTS that process afferent input from satiety signals such as CCK. Input from descending, leptin--sensitive hypothalamic projections is integrated in the NTS with vagally mediated input from CCK
anorexigenic pathways
Arcuate a-MSH, CART neurons reduce feeding behavior and energy utilization also via two pathways 1. Inhibits lateral hypothalamus to reduce appetite and food intake 2. Stimulates Paraventricular nucleus (PVN) which normally facilitates energy utilization and weight loss by increasing: -- Cortisol (from the HPA axis) which generates and mobilizes glucose -- Thyroid hormones which increases metabolic rate and oxygen utilization -- Sympathetic activity which increases lypolysis in adipose tissue
orexigenic pathways
Arcuate neurons using NPY & AgRP stimulate appetite, eating and energy storage (weight gain) via two pathways 1. Activates lateral hypothalamus which stimulates feeding related activity via: -- Vagal parasympathetic nervous system for GI digestion & motility --Brain stem centers for simple feeding behaviors (chewing). -- Cerebral cortex (prefrontal, parietal taste area, limbic) for complex feeding behaviors 2. Inhibits PVN nucleus to decrease energy utilization and promote weight gain
upper satiety signals
CCK - promotes satiety--anorexigenic CCK slows gastric emptying, releases bile, stimulates pancreatic secretion, increases intestine peristalsis
gastric satiety signals
Distension of stomach stimulates vagus nerve that projects to solitary nucleus (NTS) which activates anorexigenic hypothalamic nuclei
other hormonal effects
Leptin also regulates anterior pituitary secretion of hormones: growth hormone (GH), thyroid hormone (TH), adrenocortico- tropic hormone (ACTH) -Growth hormone increases lipolysis -Thyroid hormone increase metabolic rate and increases oxygen utilization -ACTH stimulate cortisol release from adrenal cortex & increase blood glucose levels Estrogen enhances hypothalamic responses to satiety effects of leptin, i.e. it augments satiety
anorexigenic neurons
activate pathways that inhibit eating, increase energy utilization & promote weight loss using: -CART: cocaine and amphetamine regulated transcript -α-MSH (Melanocyte stimulating hormone) released by POMC cells
orexigenic neurons
activate pathways that stimulate eating & weight gain using: - NYP (neuropeptide Y) -AgRP (Agouti-related peptide)
CCK as a satiety signal
acts on: -Vagus nerve sensory neurons projecting to solitary nucleus (NTS) which activates anorexigenic hypothalamic nuclei -NTS neurons that project to anorexic systems to limit meal size by reducing appetite and increasing sense of fullness & malaise
satiety (purpose)
acts to prevent overconsumption of food before GI is overwhelmed and cannot maintain homeostasis
many variables
are what play into determining the relative levels of food intake (eating) and energy expenditure (physical activity)
meals
based on habit, time of day, stress, i.e. factors unrelated to energy needs
energy intake and expenditure
can be determined by either homeostatic or non-homeostatic mechanisms
limbic activity
can reshape eating patterns based on associations & conditioning formed in past experiences and psychopathology (eg, depression) and are not necessarily related to energy homeostasis (anorexia, obesity)
feedback signals
come in 3 types: -Hunger & eating signals from the GI tract -Short term satiety & meal cessation signals from the GI tract -Long term adiposity signals from adipose and pancreas that modulate effects of short term satiety signals
satiety
complex sense mediated by several peptides, each elicited by specific nutrients -CCK by proteins and fats -GLP--1 by carbohydrates and fats -PYY by fat
brain stem and hypothalamic centers for energy homeostasis
controlled by peripheral signals from: -adipose tissue -pancreas -gastrointestinal tract Signals stimulate: -Vagus nerve sensory neurons directly -Solitary nucleus in brain stem -Hypothalamic nuclei
Motivation and drive in eating
determined by the limbic system
hypothalamus
intercommunicates with the limbic system to regulate eating behavior
Non-homeostatic regulation of energy
involves cognition, motivation, drive, stress- i.e. the limbic system's processing of environment, early life events, predispositions, etc.
amygdala, nucleus accumbens, and prefrontal cortex
major centers of GI conditioning
body weight (adiposity)
normally stabilized by balancing energy intake and energy expenditure (homeostasis)
eating
not based on low glucose levels (energy deficit) but on appetite/hunger
arcuate nucleus
nucleus has two populations of neurons using different transmitters 1. anorexigenic 2. orexigenic
Leptin & insulin resistance
obesity lowers transport of leptin (and insulin) into arcuate nucleus reducing satiety effect
hypothalamus and limbic system
primarily responsible for the energy balance and act via brain stem (hindbrain) to control visceral functions plus motivation and behavior
orexigenic and anorexigenic pathways
project to limbic and autonomic nuclei to regulate feeding and appetite
VTA (ventral tegmental area)
projects dopamine neurons to accumbens & prefrontal cortex as part of reward/motivation system
DMV (dorsal motor nucleus of vagus)
projects preganglionic parasympathtic neurons to adipose via the vagus nerve -Anabolically increases insulin mediated glucose uptake and FFA metabolism -Increases release of leptin
IML (intermediolateral column)
projects sympathetic activity to adipose -catabolically increases lipolysis -this is the primary role generated by anorexigenic hypothalamic pathways
neural and endocrine afferent pathways
provide feedback for regulating neural and behavioral aspects of eating
peripheral signals
provide feedback to the hypothalamus via two routes 1. Neural route 2. endocrine route
long term regulation of feeding
provided by leptin and insulin, occurs via negative feedback of appetite and feeding (other satiety signals regulate appetite on a meal by meal basis)
efferent pathways
regulate feeding behavior (food intake), appetite and satiety, plus adipose and endocrine pancreatic activity
timing of meal termination
regulated by changes in body fat content. -The efficiency of satiety signals to terminate a meal varies with amount of body fat as signaled by insulin and leptin -Overeating increases fat levels which raise leptin levels. -Either leptin enhances sensitivity to satiety signals OR leptin resistance develops and maintains adiposity at a new equilibrium point
stomach, upper GI & lower GI
release satiety signals
endocrine route (peripheral signals)
released from GI act on hypothalamic nuclei
hunger signal
released from oxyntic stomach glands
satiety signals
shift hypothalamic activity to anorectic state by: Stimulating anorexigenic, α-MMSSHH,, CART nuclei Inhibiting orexigenic NPY, AgRP nuclei
ghrelin
stimulates eating - orexigenic -Stimulates NPY/AgRP pathways and brain stem parasympathetic nuclei to promote eating & GI secretions -Stimulates ventral tegmentum dopamine path to n. accumbens to increase motivation to eat -Impacts limbic system (amygdala & hippocampus) to form memory of food
arcuate, paraventricular & lateral hypothalamic nuclei
the primary hypothalamic nuclei that regulate feeding behavior (appetite, satiety, meal size, etc)
homeostatic regulation of energy
the result of feedback regulation from the internal milieu (adipose, intestines, pancreas, etc) on hypothalamic/brain stem actions on eating
when leptin and insulin are working TOGETHER
their net effect is to: -inhibit eating (via LH) by changing sensitivity to satiety signals -Increase energy utilization (PVN ----mobilize glucose and fat ----increased oxygen consumption and higher body temperature leads to loss of fat tissue
arcuate nucleus
where leptin & insulin bind to reduce appetite and fat deposition by: -stimulating anorexigenic CART/α-MSH pathway -inhibit orexigenic NPY/AgRP path
