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The Brain's Hunger/Satiety Pathways and Obesity, Animation
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The Brain's Hunger/Satiety Pathways and Obesity, Animation

Food Intake and Energy Balance

This section discusses the balance between food intake and energy expenditure in maintaining a healthy body weight. The central nervous system, particularly the brainstem and hypothalamus, plays a crucial role in controlling feeding behavior and energy metabolism.

Brain Systems Involved in Energy Balance

  • The central nervous system, specifically the brainstem and hypothalamus, controls feeding behavior and energy metabolism.
  • The brainstem receives neuronal inputs from the digestive tract, while the hypothalamus picks up hormonal and nutritional signals from the circulation.
  • These systems collect information about nutrient status and interact with reward and motivation pathways that drive food-seeking behavior.

Appetite Control in the Hypothalamus

  • The arcuate nucleus (ARC) of the hypothalamus is a major control center for appetite regulation. It contains two groups of neurons with opposing functions: appetite-stimulating neurons expressing NPY and AGRP peptides, and appetite-suppressing neurons producing POMC peptide.
  • Hunger activates appetite-stimulating neurons, while satiety stimulates appetite-suppressing neurons.
  • Neurons from the ARC project to other nuclei of the hypothalamus, particularly the paraventricular nucleus (PVN), which further processes information to coordinate a response controlling energy intake and expenditure.

Short-term Regulation of Feeding

  • Short-term regulation of feeding depends on stomach fullness and nutrient presence in the intestine. An empty stomach signals hunger to the brainstem through stretch information, while ghrelin production stimulates feeding by acting on the ARC.
  • Food ingestion leads to stomach distension perceived as satiety by the brainstem. Ghrelin production stops, and other gut peptides are released to suppress appetite and increase energy expenditure.

Long-term Regulation of Feeding

  • Long-term regulation of feeding is influenced by body fat content. Low body fat encourages feeding and energy preservation, while high body fat suppresses appetite and promotes energy expenditure.
  • Leptin and insulin are two hormones involved in long-term regulation. Leptin, secreted by adipose tissues, signals the brain about sufficient energy storage, leading to reduced food intake and increased energy expenditure. Insulin, released upon food ingestion, also plays a role in regulating feeding behaviors.

Factors Contributing to Obesity

  • Obesity results from dysregulation of feeding behaviors and energy metabolism. Chronic low leptin activities are commonly associated with obesity as they trick the brain into perceiving starvation, leading to overeating and excessive fat storage.
  • Both genetic factors and lifestyle choices contribute to low leptin signaling. A high-fat diet is a major lifestyle factor that affects leptin signaling by inducing inflammation in hypothalamic neurons, resulting in leptin resistance.
  • Genetic factors include mutations in the leptin gene itself or downstream genes required for proper leptin action in various pathways. Maternal obesity and a high-fat diet during pregnancy are risk factors for childhood obesity.
Video description

(USMLE topics, neurobiology) The appetite pathway in the brain, leptin, and pathology of obesity. Purchase a license to download a non-watermarked version of this video on AlilaMedicalMedia(dot)com Check out our new Alila Academy - AlilaAcademy(dot)com - complete video courses with quizzes, PDFs, and downloadable images. ©Alila Medical Media. All rights reserved. Voice by: Ashley Fleming All images/videos by Alila Medical Media are for information purposes ONLY and are NOT intended to replace professional medical advice, diagnosis or treatment. Always seek the advice of a qualified healthcare provider with any questions you may have regarding a medical condition. Food intake and energy expenditure must be balanced to maintain a healthy body weight. This balance is kept by the central nervous system, which controls feeding behavior and energy metabolism. Several brain systems are involved, including the brainstem which receives neuronal inputs from the digestive tract, and the hypothalamus which picks up hormonal and nutritional signals from the circulation. They also interact with the reward and motivation pathways, which drive food-seeking behavior. The arcuate nucleus, ARC, of the hypothalamus: two groups of neurons, with opposing functions, in the ARC: the appetite-stimulating neurons expressing NPY and AGRP peptides, and the appetite-suppressing neurons producing POMC peptide. Neurons of the ARC project to other nuclei of the hypothalamus, of which the paraventricular nucleus, PVN, is most important. PVN neurons further process the information and project to other circuits outside the hypothalamus, thus coordinating a response that controls energy intake and expenditure. Short-term regulation of feeding is based on how empty or how full the stomach is, and if there are nutrients in the intestine. In the fasting state, an empty stomach sends stretch information to the brainstem, signaling hunger. It produces a peptide called ghrelin, which acts on the arcuate nucleus to stimulate feeding. Ghrelin also acts directly on the PVN to reduce energy expenditure. Upon food ingestion, distension of the stomach is perceived by the brainstem as satiety. Several other gut peptides are released from the intestine and act on the hypothalamus and other brain areas to suppress appetite and increase energy expenditure. Long-term regulation takes cues from the amount of body fat: low body fat content encourages feeding and energy preservation, while high body fat suppresses appetite and promotes energy expenditure. Two hormones are involved: leptin and insulin. Insulin is a hormone produced by the pancreas and is released into the bloodstream upon food ingestion, when blood glucose starts to rise. Leptin is a hormone secreted by adipose tissues in a process dependent on insulin. The amount of circulating leptin in the plasma is directly proportional to the body fat content. Increased leptin levels in the blood signal to the brain that the body has enough energy storage, and that it has to stop eating and burn more energy. Leptin and insulin seem to work together on hypothalamic nuclei, as well as other brain areas, to inhibit food intake and increase energy expenditure. Obesity results from the dysregulation of feeding behaviors and energy metabolism. Obesity is associated with chronic low leptin activities, which trick the brain into thinking that the body is always starved. This leads to overeating and excessive energy storage as fats. The major lifestyle factor is a high-fat, energy-rich diet. In an early stage of high-fat-diet–induced obesity, increased amounts of saturated fatty acids cross the blood brain barrier and provoke an inflammatory response in hypothalamic neurons. Inflammation induces stress in these neurons, blunting their response to leptin. This is known as leptin resistance. Leptin levels are high, but because the cells cannot react to leptin, the brain interprets it as low and triggers the starvation response. Genetic factors include mutations in the leptin gene itself, or in one of the numerous downstream genes that are required for leptin action in various pathways. Leptin deficiency due to gene mutations is very rare. More common are mutations in the downstream genes, which render a certain pathway irresponsive to leptin. A major risk factor for childhood obesity is maternal obesity and mother’s high-fat-diet during pregnancy and lactation. A maternal diet rich in saturated fats can cause inflammation in the infant’s hypothalamus. It may also prime the reward pathways in infants, influencing their food choice toward energy-rich foods.