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Carbohydrate Metabolism

Carbohydrate Metabolism. METABOLISM? WHY?. A 59-year-old man with a history of diabetes and alcohol abuse is brought to the emergency room in a semiconscious and minimally responsive state How are glucose, triacylglycerols , and amino acids normally metabolized and what happens in diabetes?.

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Carbohydrate Metabolism

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  1. Carbohydrate Metabolism

  2. METABOLISM? WHY? • A 59-year-old man with a history of diabetes and alcohol abuse is brought to the emergency room in a semiconscious and minimally responsive state • How are glucose, triacylglycerols, and amino acids normally metabolized and what happens in diabetes?

  3. Major Pathways 1. Glycolysis 2. Citric acid cycle 3. Gluconeogenesis 4. Glycogen metabolism (a) Glycogenesis (b) Glycogenolysis

  4. Glucose • Glucose is the most important carbohydrate • Glucose is the major metabolic fuel of mammals. • Monosaccharide from diet : - Glucose - Fructose - Galactose • Fructose and Galactose glucose at the liver

  5. Glucose at the center of metabolism Ketone bodies Glucose Fatty acids (TGA) Glycogen Glycolysis Glycogenolysis G6P β-Oxidation Glycogenesis Lipogenesis Lipolysis Gluconeogenesis Lactate Pyruvate Acetyl-CoA Electron Transport Chain Amino acids (Protein) Krebs cycle

  6. Major organ of metabolism Glycogenesis Glycogenolysis Lipogenesis Lipolysis β-Oxidation Glycogenesis Glycogenolysis Gluconeogenesis Lipogenesis Lipolysis β-Oxidation Ketogenesis Blood Glucose Serum Triglycerides Glycogenesis Glycogenolysis Glycolysis β-Oxidation Glycogenesis Glycogenolysis Glycolysis β-Oxidation

  7. The origine of glucose Fats Aminoacids monosaccharide GLUCOSE Glycogen Exogenous

  8. Glucose Homeostasis

  9. The fate of glucose

  10. Glycolysis

  11. Krebs Cycle

  12. Integration of metabolism • Common intermediates • Common organs

  13. The metabolicintermediates. Metabolicintegration

  14. Major organ of metabolism, metabolicintegration Glycogenesis Glycogenolysis Lipogenesis Lipolysis β-Oxidation Glycogenesis Glycogenolysis Gluconeogenesis Lipogenesis Lipolysis β-Oxidation Ketogenesis Blood Glucose Serum Triglycerides Glycogenesis Glycogenolysis Glycolysis β-Oxidation Glycogenesis Glycogenolysis Glycolysis β-Oxidation

  15. Glucose, in between organ currency

  16. Regulation of Blood Glucose: Insulin • Insulin • Produced by beta cells of the pancreas • Helps transport glucose from the blood into cells • Stimulates the liver to take up glucose and convert it to glycogen

  17. Regulation of Blood Glucose: Insulin

  18. Insulin

  19. Regulation of Blood Glucose: Glucagon • Glucagon • Produced by alpha cells of the pancreas • Stimulates the breakdown of glycogen to glucose to make glucose available to cells of the body • Stimulates gluconeogenesis—the production of “new” glucose from amino acids

  20. Regulation of Blood Glucose: Glucagon

  21. Glucangon

  22. Insulin, Glucagon, and blood glucose

  23. Blood glocose • High Blood glucose 1. Glycolysis 2. Glycogenesis 3. HMP Shunt 4. Oxidation of Pyruvate 5. Kreb’s Cycle 6. Change to lipids • Low blood glucose 1. Glycogenolysis 2. Gluconeogenesis

  24. Gluconeogenesis

  25. Overview of Glucose Metabolism

  26. glycolysis gluconeogenesis sugar (re)new create gluco neo genesis glucose pyruvate lactate

  27. Topics: Gluconeogenesis • Principles, substrates & relationship to glycolysis • Bypass of irreversible steps in glycolysis • Link between liver gluconeogenesis and muscle/RBC/brain glycolysis; the Cori and Alanine cycles

  28. Gluconeogenesis • Occurs in all animals, plants, fungi and microbes • Occurs largely in the liver; some in renal cortex • Of 10 enzymatic steps, 7 are reversals of glycolytic reactions

  29. Metabolites feed into gluconeogenesis at various points main path

  30. AA can feed into gluconeogenesis

  31. TCA intermediates are gluconeogenic;funnel through oxaloacetate

  32. Bypass of irreversible steps in glycolysis

  33. Irreversible glycolytic stepsbypassed glycolysis gluconeogenesis by Glucose-6-phosphatase by Fructose 1,6-bisphosphatase (FBP-1) by Pyruvate Carboxylase & Phosphoenolpyruvate carboxykinase (PEPCK) • Hexokinase (hexK) • Phosphofructokinase-1 (PFK-1) • Pyruvate kinase (PyrK) These 3 key enzymes

  34. Pyruvate can go “up” or “down” depending upon energy needs

  35. First bypass step is generation of PEP from pyruvate via oxaloacetate • *Note: • In order to cross the mito membrane, oxaloacetate must: • Be reduced to malate • Go through the malate shuttle • Be reoxidized to oxaloacetate

  36. Addition of CO2 to pyruvate to form oxaloacetate • Hydrolysis of ATP

  37. Decarboxylation and phosphorylation to PEP

  38. 2nd & 3rd bypass steps are near the end of gluconeogenesis(“top” of glycolysis) Regulation of FBP-1 by AMP and F2,6P

  39. Dephosphorylation of G6P,3rd bypass reaction

  40. Glucose 6-phosphatase removes the phosphate to liberate free glucose G6Pase glucose-6-P + H2O  glucose + Pi • This is primarily a function of the liver to buffer blood glucose levels • G6Pase is NOT present in brain and muscle! (Gluconeogenesis does not occur in these tissues)

  41. cost Gluconeogenesis is energetically expensive to cells (hepatocytes)

  42. Note that both Glycolysis and Gluconeogenesis are energetically favorable under physiological conditions and therefore both ~ irreversible processes GlycolysisDG[phys] = -63 kJ/mol GluconeogenesisDG[phys] = -16 kJ/mol

  43. Liver is the major source of blood glucose from GN Is the primary gluconeogenic organ Produces glucose for export to brain, muscle, RBC’s Uses many small metabolites and fatty acids to feed GN Liver function is highly sensitive to insulin & glucagon

  44. The Cori Cycle Lactate and glucose shuttle between active muscle/RBC and liver (glucagon/insulin reg.) Liver gluconeogenesis buffers the blood glucose for use by muscle, RBC’s and brain (120 g/day) *Note: the brain fully oxidizes glucose, so it does not funnel back lactate GN 6 ATP 2 RBCs 2 ATP GL

  45. The Alanine Cycle The liver can also use the amino acid Alanine similarly to Lactate Following transamination to pyruvate, gluconeogenesis allows the liver to convert it to glucose for secretion into the blood

  46. Regulation of Gluconeogenesis

  47. First Coordinated Control Point 1. high energy charge or abundance of biosynthetic intermediates turn off glycolysis.. Glycolytic pathway intermediate turns it on (2) (1) (3) 2. when energy charge of the cell is low, the biosynthetic pathway is turned off. 3. when excess acetyl CoA builds up glucose formation is stimulated. When the energy charge in the cell is low, biosynthesis is turned off.

  48. Second Coordinated Control Point Recall that F-2,6-BP is a signal molecule that is present at low concentration during starvation and high concentration in the fed state due to the antagonistic effects of glucagon and insulin on its production.

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