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Glucagon

February 15, 2024

This article is about the natural hormone. For the medication, see Glucagon (medication).

Glucagon is a peptide hormone, produced by alpha cells of the pancreas. It raises the concentration of glucose and fatty acids in the bloodstream and is considered to be the main catabolic hormone of the body.[1] It is also used as a medication to treat a number of health conditions. Its effect is opposite to that of insulin, which lowers extracellular glucose.[2] It is produced from proglucagon, encoded by the GCG gene.

glucagon
Identifiers
AliasesGCG(53-81)glucagoneglucagon recombinant
External IDsGeneCards: [1]
Orthologs
SpeciesHumanMouse
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UniProt

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View/Edit Human

The pancreas releases glucagon when the amount of glucose in the bloodstream is too low. Glucagon causes the liver to engage in glycogenolysis: converting stored glycogen into glucose, which is released into the bloodstream.[3] High blood-glucose levels, on the other hand, stimulate the release of insulin. Insulin allows glucose to be taken up and used by insulin-dependent tissues. Thus, glucagon and insulin are part of a feedback system that keeps blood glucose levels stable. Glucagon increases energy expenditure and is elevated under conditions of stress.[4] Glucagon belongs to the secretin family of hormones.

Structure edit

Glucagon is a 29-amino acid polypeptide. Its primary structure in humans is: NH2-His-Ser-Gln-Gly-Thr-Phe-Thr-Ser-Asp-Tyr-Ser-Lys-Tyr-Leu-Asp-Ser-Arg-Arg-Ala-Gln-Asp-Phe-Val-Gln-Trp-Leu-Met-Asn-Thr-COOH (HSQGTFTSDYSKYLDSRRAQDFVQWLMNT).

The polypeptide has a molecular mass of 3485 daltons.[5] Glucagon is a peptide (nonsteroid) hormone.

Physiology edit

Production edit

 
A microscopic image stained for glucagon

The hormone is synthesized and secreted from alpha cells (α-cells) of the islets of Langerhans, which are located in the endocrine portion of the pancreas. Glucagon is produced from the preproglucagon gene Gcg. Preproglucagon first has its signal peptide removed by signal peptidase, forming the 160-amino acid protein proglucagon.[6] Proglucagon is then cleaved by proprotein convertase 2 to glucagon (amino acids 33-61) in pancreatic islet α cells. In intestinal L cells, proglucagon is cleaved to the alternate products glicentin (1–69), glicentin-related pancreatic polypeptide (1–30), oxyntomodulin (33–69), glucagon-like peptide 1 (72–107 or 108), and glucagon-like peptide 2 (126–158).[6]

In rodents, the alpha cells are located in the outer rim of the islet. Human islet structure is much less segregated, and alpha cells are distributed throughout the islet in close proximity to beta cells. Glucagon is also produced by alpha cells in the stomach.[7]

Recent research has demonstrated that glucagon production may also take place outside the pancreas, with the gut being the most likely site of extrapancreatic glucagon synthesis.[8]

Regulation edit

Production, which is otherwise freerunning, is suppressed/regulated by amylin, a peptide hormone co-secreted with insulin from the pancreatic β cells.[9] As plasma glucose levels recede, the subsequent reduction in amylin secretion alleviates its suppression of the α cells, allowing for glucagon secretion.

Secretion of glucagon is stimulated by:

Secretion of glucagon is inhibited by:

Function edit

Glucagon generally elevates the concentration of glucose in the blood by promoting gluconeogenesis and glycogenolysis.[17] Glucagon also decreases fatty acid synthesis in adipose tissue and the liver, as well as promoting lipolysis in these tissues, which causes them to release fatty acids into circulation where they can be catabolised to generate energy in tissues such as skeletal muscle when required.[18]

Glucose is stored in the liver in the form of the polysaccharide glycogen, which is a glucan (a polymer made up of glucose molecules). Liver cells (hepatocytes) have glucagon receptors. When glucagon binds to the glucagon receptors, the liver cells convert the glycogen into individual glucose molecules and release them into the bloodstream, in a process known as glycogenolysis. As these stores become depleted, glucagon then encourages the liver and kidney to synthesize additional glucose by gluconeogenesis. Glucagon turns off glycolysis in the liver, causing glycolytic intermediates to be shuttled to gluconeogenesis.

Glucagon also regulates the rate of glucose production through lipolysis. Glucagon induces lipolysis in humans under conditions of insulin suppression (such as diabetes mellitus type 1).[19]

Glucagon production appears to be dependent on the central nervous system through pathways yet to be defined. In invertebrate animals, eyestalk removal has been reported to affect glucagon production. Excising the eyestalk in young crayfish produces glucagon-induced hyperglycemia.[20]

Mechanism of action edit

 
Metabolic regulation of glycogen by glucagon.

Glucagon binds to the glucagon receptor, a G protein-coupled receptor, located in the plasma membrane of the cell. The conformation change in the receptor activates a G protein, a heterotrimeric protein with αs, β, and γ subunits. When the G protein interacts with the receptor, it undergoes a conformational change that results in the replacement of the GDP molecule that was bound to the α subunit with a GTP molecule.[21] This substitution results in the releasing of the α subunit from the β and γ subunits. The alpha subunit specifically activates the next enzyme in the cascade, adenylate cyclase.

Adenylate cyclase manufactures cyclic adenosine monophosphate (cyclic AMP or cAMP), which activates protein kinase A (cAMP-dependent protein kinase). This enzyme, in turn, activates phosphorylase kinase, which then phosphorylates glycogen phosphorylase b (PYG b), converting it into the active form called phosphorylase a (PYG a). Phosphorylase a is the enzyme responsible for the release of glucose 1-phosphate from glycogen polymers. An example of the pathway would be when glucagon binds to a transmembrane protein. The transmembrane proteins interacts with Gɑβ𝛾. Gαs separates from Gβ𝛾 and interacts with the transmembrane protein adenylyl cyclase. Adenylyl cyclase catalyzes the conversion of ATP to cAMP. cAMP binds to protein kinase A, and the complex phosphorylates glycogen phosphorylase kinase.[22] Phosphorylated glycogen phosphorylase kinase phosphorylates glycogen phosphorylase. Phosphorylated glycogen phosphorylase clips glucose units from glycogen as glucose 1-phosphate.

Additionally, the coordinated control of glycolysis and gluconeogenesis in the liver is adjusted by the phosphorylation state of the enzymes that catalyze the formation of a potent activator of glycolysis called fructose 2,6-bisphosphate.[23] The enzyme protein kinase A (PKA) that was stimulated by the cascade initiated by glucagon will also phosphorylate a single serine residue of the bifunctional polypeptide chain containing both the enzymes fructose 2,6-bisphosphatase and phosphofructokinase-2. This covalent phosphorylation initiated by glucagon activates the former and inhibits the latter. This regulates the reaction catalyzing fructose 2,6-bisphosphate (a potent activator of phosphofructokinase-1, the enzyme that is the primary regulatory step of glycolysis)[24] by slowing the rate of its formation, thereby inhibiting the flux of the glycolysis pathway and allowing gluconeogenesis to predominate. This process is reversible in the absence of glucagon (and thus, the presence of insulin).

Glucagon stimulation of PKA inactivates the glycolytic enzyme pyruvate kinase,[25] inactivates glycogen synthase,[26] and activates hormone-sensitive lipase,[27] which catabolizes glycerides into glycerol and free fatty acid(s), in hepatocytes.

Glucagon also inactivates acetyl-CoA carboxylase, which creates malonyl-CoA from acetyl-CoA, through cAMP-dependent and/or cAMP-independent kinases.[28]

Malonyl-CoA is a byproduct of the Krebs cycle (downstream of glycolysis) and an allosteric inhibitor of Carnitine palmitoyltransferase I (CPT1), a mitochondrial enzyme important for bringing fatty acids into the intermembrane space of the mitochondria for β-oxidation.[29] Glucagon decreases malonyl-CoA through inhibition of acetyl-CoA carboxylase and through reduced glycolysis through its aforementioned reduction in Fructose 2,6-bisphosphate. Thus, reduction in malonyl-CoA is a common regulator for the increased fatty acid metabolism effects of glucagon.

Pathology edit

Abnormally elevated levels of glucagon may be caused by pancreatic tumors, such as glucagonoma, symptoms of which include necrolytic migratory erythema,[30] reduced amino acids, and hyperglycemia. It may occur alone or in the context of multiple endocrine neoplasia type 1.[31]

Elevated glucagon is the main contributor to hyperglycemic ketoacidosis in undiagnosed or poorly treated type 1 diabetes. As the beta cells cease to function, insulin and pancreatic GABA are no longer present to suppress the freerunning output of glucagon. As a result, glucagon is released from the alpha cells at a maximum, causing a rapid breakdown of glycogen to glucose and fast ketogenesis .[32] It was found that a subset of adults with type 1 diabetes took 4 times longer on average to approach ketoacidosis when given somatostatin (inhibits glucagon production) with no insulin.[citation needed] Inhibiting glucagon has been a popular idea of diabetes treatment, however, some have warned that doing so will give rise to brittle diabetes in patients with adequately stable blood glucose.[citation needed]

The absence of alpha cells (and hence glucagon) is thought to be one of the main influences in the extreme volatility of blood glucose in the setting of a total pancreatectomy.

History edit

In the early 1920s, several groups noted that pancreatic extracts injected into diabetic animals would result in a brief increase in blood sugar prior to the insulin-driven decrease in blood sugar.[6] In 1922, C. Kimball and John R. Murlin identified a component of pancreatic extracts responsible for this blood sugar increase, terming it "glucagon", a portmanteau of "glucose agonist".[6][33] In the 1950s, scientists at Eli Lilly isolated pure glucagon, crystallized it, and determined its amino acid sequence.[6][34][35] This led to the development of the first radioimmunoassay for detecting glucagon, described by Roger Unger's group in 1959.[6]

A more complete understanding of its role in physiology and disease was not established until the 1970s, when a specific radioimmunoassay was developed.[36]

See also edit

References edit

  1. ^ Voet D, Voet JG (2011). Biochemistry (4th ed.). New York: Wiley.
  2. ^ Reece J, Campbell N (2002). Biology. San Francisco: Benjamin Cummings. ISBN 978-0-8053-6624-2.
  3. ^ Orsay J (2014). Biology 1: Molecules. Examkrackers Inc. p. 77. ISBN 978-1-893858-70-1.
  4. ^ Jones BJ, Tan T, Bloom SR (March 2012). "Minireview: Glucagon in stress and energy homeostasis". Endocrinology. 153 (3): 1049–54. doi:10.1210/en.2011-1979. PMC 3281544. PMID 22294753.
  5. ^ Unger RH, Orci L (June 1981). "Glucagon and the A cell: physiology and pathophysiology (first two parts)". The New England Journal of Medicine. 304 (25): 1518–24. doi:10.1056/NEJM198106183042504. PMID 7015132.
  6. ^ a b c d e f Müller TD, Finan B, Clemmensen C, DiMarchi RD, Tschöp MH (April 2017). "The New Biology and Pharmacology of Glucagon". Physiol Rev. 97 (2): 721–766. doi:10.1152/physrev.00025.2016. PMID 28275047.
  7. ^ Unger RH, Cherrington AD (January 2012). "Glucagonocentric restructuring of diabetes: a pathophysiologic and therapeutic makeover". The Journal of Clinical Investigation. 122 (1): 4–12. doi:10.1172/JCI60016. PMC 3248306. PMID 22214853.
  8. ^ Holst JJ, Holland W, Gromada J, Lee Y, Unger RH, Yan H, Sloop KW, Kieffer TJ, Damond N, Herrera PL (April 2017). "Insulin and Glucagon: Partners for Life". Endocrinology. 158 (4): 696–701. doi:10.1210/en.2016-1748. PMC 6061217. PMID 28323959.
  9. ^ a b Zhang XX, Pan YH, Huang YM, Zhao HL (May 2016). "Neuroendocrine hormone amylin in diabetes". World Journal of Diabetes. 7 (9): 189–197. doi:10.4239/wjd.v7.i9.189. PMC 4856891. PMID 27162583.
  10. ^ Layden BT, Durai V, Lowe WL (2010). "G-Protein-Coupled Receptors, PANCREATIC Islets, and DiAbetes". Nature Education. 3 (9): 13.
  11. ^ Skoglund G, Lundquist I, Ahrén B (November 1987). "Alpha 1- and alpha 2-adrenoceptor activation increases plasma glucagon levels in the mouse". European Journal of Pharmacology. 143 (1): 83–8. doi:10.1016/0014-2999(87)90737-0. PMID 2891547.
  12. ^ Honey RN, Weir GC (October 1980). "Acetylcholine stimulates insulin, glucagon, and somatostatin release in the perfused chicken pancreas". Endocrinology. 107 (4): 1065–8. doi:10.1210/endo-107-4-1065. PMID 6105951.
  13. ^ REHFELD, JENS (February 1978). "The effect of gastrin on basal and aminoacid-stimulated insulin and glucagon secretion in man". European Journal of Clinical Investigation. 8 (1): 5–9. doi:10.1111/j.1365-2362.1978.tb00800.x. PMID 417933. S2CID 38154468.
  14. ^ Xu E, Kumar M, Zhang Y, Ju W, Obata T, Zhang N, Liu S, Wendt A, Deng S, Ebina Y, Wheeler MB, Braun M, Wang Q (January 2006). "Intra-islet insulin suppresses glucagon release via GABA-GABAA receptor system". Cell Metabolism. 3 (1): 47–58. doi:10.1016/j.cmet.2005.11.015. PMID 16399504.
  15. ^ Krätzner R, Fröhlich F, Lepler K, Schröder M, Röher K, Dickel C, Tzvetkov MV, Quentin T, Oetjen E, Knepel W (February 2008). "A peroxisome proliferator-activated receptor gamma-retinoid X receptor heterodimer physically interacts with the transcriptional activator PAX6 to inhibit glucagon gene transcription". Molecular Pharmacology. 73 (2): 509–17. doi:10.1124/mol.107.035568. PMID 17962386. S2CID 10108970.
  16. ^ Johnson LR (2003). Essential Medical Physiology. Academic Press. pp. 643–. ISBN 978-0-12-387584-6.
  17. ^ Voet D, Voet JG (2011). Biochemistry (4th ed.). New York: Wiley.
  18. ^ Habegger KM, Heppner KM, Geary N, Bartness TJ, DiMarchi R, Tschöp MH (December 2010). "The metabolic actions of glucagon revisited". Nature Reviews. Endocrinology. 6 (12): 689–697. doi:10.1038/nrendo.2010.187. PMC 3563428. PMID 20957001.
  19. ^ Liljenquist JE, Bomboy JD, Lewis SB, Sinclair-Smith BC, Felts PW, Lacy WW, Crofford OB, Liddle GW (January 1974). "Effects of glucagon on lipolysis and ketogenesis in normal and diabetic men". The Journal of Clinical Investigation. 53 (1): 190–7. doi:10.1172/JCI107537. PMC 301453. PMID 4808635.
  20. ^ Leinen RL, Giannini AJ (1983). "Effect of eyestalk removal on glucagon induced hyperglycemia in crayfish". Society for Neuroscience Abstracts. 9: 604.
  21. ^ "Glucagon Signaling Pathway". News-Medical.net. 2018-03-01. Retrieved 2021-03-30.
  22. ^ Yu Q, Shuai H, Ahooghalandari P, Gylfe E, Tengholm A (July 2019). "Glucose controls glucagon secretion by directly modulating cAMP in alpha cells". Diabetologia. 62 (7): 1212–1224. doi:10.1007/s00125-019-4857-6. PMC 6560012. PMID 30953108.
  23. ^ Hue L, Rider MH (July 1987). "Role of fructose 2,6-bisphosphate in the control of glycolysis in mammalian tissues". The Biochemical Journal. 245 (2): 313–24. doi:10.1042/bj2450313. PMC 1148124. PMID 2822019.
  24. ^ Claus TH, El-Maghrabi MR, Regen DM, Stewart HB, McGrane M, Kountz PD, Nyfeler F, Pilkis J, Pilkis SJ (1984). The Role of Fructose 2,6-Bisphosphate in the Regulation of Carbohydrate Metabolism. Current Topics in Cellular Regulation. Vol. 23. pp. 57–86. doi:10.1016/b978-0-12-152823-2.50006-4. ISBN 9780121528232. PMID 6327193.
  25. ^ Feliú JE, Hue L, Hers HG (August 1976). "Hormonal control of pyruvate kinase activity and of gluconeogenesis in isolated hepatocytes". Proceedings of the National Academy of Sciences of the United States of America. 73 (8): 2762–6. Bibcode:1976PNAS...73.2762F. doi:10.1073/pnas.73.8.2762. PMC 430732. PMID 183209.
  26. ^ Jiang G, Zhang BB (April 2003). "Glucagon and regulation of glucose metabolism". Am J Physiol Endocrinol Metab. 284 (4): E671-8. doi:10.1152/ajpendo.00492.2002. PMID 12626323.
  27. ^ Hayashi Y (January 2021). "Glucagon regulates lipolysis and fatty acid oxidation through inositol triphosphate receptor 1 in the liver". Diabetes Investig. 12 (1): 32–34. doi:10.1111/jdi.13315. PMC 7779274. PMID 32506830.
  28. ^ Swenson TL, Porter JW (Mar 25, 1985). "Mechanism of glucagon inhibition of liver acetyl-CoA carboxylase. Interrelationship of the effects of phosphorylation, polymer-protomer transition, and citrate on enzyme activity". The Journal of Biological Chemistry. 2460 (6): 3791–3797. doi:10.1016/S0021-9258(19)83693-1. PMID 2857722.
  29. ^ Wang Y, Yu W, Li S, Guo D, He J, Wang Y (March 11, 2022). "Acetyl-CoA Carboxylases and Diseases". Frontiers in Oncology. 12. doi:10.3389/fonc.2022.836058. PMC 8963101. PMID 35359351.
  30. ^ John AM, Schwartz RA (December 2016). "Glucagonoma syndrome: a review and update on treatment". Journal of the European Academy of Dermatology and Venereology. 30 (12): 2016–2022. doi:10.1111/jdv.13752. PMID 27422767. S2CID 1228654.
  31. ^ Oberg K (December 2010). "Pancreatic endocrine tumors". Seminars in Oncology. 37 (6): 594–618. doi:10.1053/j.seminoncol.2010.10.014. PMID 21167379.
  32. ^ Fasanmade OA, Odeniyi IA, Ogbera AO (June 2008). "Diabetic ketoacidosis: diagnosis and management". African Journal of Medicine and Medical Sciences. 37 (2): 99–105. PMID 18939392.
  33. ^ Kimball C, Murlin J (1923). "Aqueous extracts of pancreas III. Some precipitation reactions of insulin". J. Biol. Chem. 58 (1): 337–348. doi:10.1016/S0021-9258(18)85474-6.
  34. ^ Staub A, Sinn L, Behrens OK (June 1953). "Purification and crystallization of hyperglycemic glycogenolytic factor (HGF)". Science. 117 (3049): 628–9. Bibcode:1953Sci...117..628S. doi:10.1126/science.117.3049.628. PMID 13056638.
  35. ^ Bromer W, Winn L, Behrens O (1957). "The amino acid sequence of glucagon V. Location of amide groups, acid degradation studies and summary of sequential evidence". J. Am. Chem. Soc. 79 (11): 2807–2810. doi:10.1021/ja01568a038.
  36. ^ Lundqvist, Gudmar; Edwards, John; Wide, Leif (January 1976). "A Solid Phase Radioimmunoassay for Pancreatic Glucagon". Upsala Journal of Medical Sciences. 81 (2): 65–69. doi:10.3109/03009737609179024. ISSN 0300-9734. PMID 785743.

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February 15, 2024
glucagon, this, article, about, natural, hormone, medication, medication, peptide, hormone, produced, alpha, cells, pancreas, raises, concentration, glucose, fatty, acids, bloodstream, considered, main, catabolic, hormone, body, also, used, medication, treat, . This article is about the natural hormone For the medication see Glucagon medication Glucagon is a peptide hormone produced by alpha cells of the pancreas It raises the concentration of glucose and fatty acids in the bloodstream and is considered to be the main catabolic hormone of the body 1 It is also used as a medication to treat a number of health conditions Its effect is opposite to that of insulin which lowers extracellular glucose 2 It is produced from proglucagon encoded by the GCG gene glucagonIdentifiersAliasesGCG 53 81 glucagoneglucagon recombinantExternal IDsGeneCards 1 RNA expression patternBgeeHumanMouse ortholog n an aBioGPSMore reference expression dataOrthologsSpeciesHumanMouseEntrezn an aEnsembln an aUniProtnan aRefSeq mRNA n an aRefSeq protein n an aLocation UCSC n an aPubMed searchn an aWikidataView Edit HumanThe pancreas releases glucagon when the amount of glucose in the bloodstream is too low Glucagon causes the liver to engage in glycogenolysis converting stored glycogen into glucose which is released into the bloodstream 3 High blood glucose levels on the other hand stimulate the release of insulin Insulin allows glucose to be taken up and used by insulin dependent tissues Thus glucagon and insulin are part of a feedback system that keeps blood glucose levels stable Glucagon increases energy expenditure and is elevated under conditions of stress 4 Glucagon belongs to the secretin family of hormones Contents 1 Structure 2 Physiology 2 1 Production 2 2 Regulation 3 Function 4 Mechanism of action 5 Pathology 6 History 7 See also 8 References 9 External linksStructure editGlucagon is a 29 amino acid polypeptide Its primary structure in humans is NH2 His Ser Gln Gly Thr Phe Thr Ser Asp Tyr Ser Lys Tyr Leu Asp Ser Arg Arg Ala Gln Asp Phe Val Gln Trp Leu Met Asn Thr COOH HSQGTFTSDYSKYLDSRRAQDFVQWLMNT The polypeptide has a molecular mass of 3485 daltons 5 Glucagon is a peptide nonsteroid hormone Physiology editProduction edit nbsp A microscopic image stained for glucagonThe hormone is synthesized and secreted from alpha cells a cells of the islets of Langerhans which are located in the endocrine portion of the pancreas Glucagon is produced from the preproglucagon gene Gcg Preproglucagon first has its signal peptide removed by signal peptidase forming the 160 amino acid protein proglucagon 6 Proglucagon is then cleaved by proprotein convertase 2 to glucagon amino acids 33 61 in pancreatic islet a cells In intestinal L cells proglucagon is cleaved to the alternate products glicentin 1 69 glicentin related pancreatic polypeptide 1 30 oxyntomodulin 33 69 glucagon like peptide 1 72 107 or 108 and glucagon like peptide 2 126 158 6 In rodents the alpha cells are located in the outer rim of the islet Human islet structure is much less segregated and alpha cells are distributed throughout the islet in close proximity to beta cells Glucagon is also produced by alpha cells in the stomach 7 Recent research has demonstrated that glucagon production may also take place outside the pancreas with the gut being the most likely site of extrapancreatic glucagon synthesis 8 Regulation edit Production which is otherwise freerunning is suppressed regulated by amylin a peptide hormone co secreted with insulin from the pancreatic b cells 9 As plasma glucose levels recede the subsequent reduction in amylin secretion alleviates its suppression of the a cells allowing for glucagon secretion Secretion of glucagon is stimulated by Hypoglycemia Epinephrine via b2 a2 10 and a1 11 adrenergic receptors Arginine Alanine often from muscle derived pyruvate glutamate transamination see alanine transaminase reaction Acetylcholine 12 Cholecystokinin Gastric inhibitory polypeptide Gastrin 13 Secretion of glucagon is inhibited by Somatostatin Amylin 9 Insulin via GABA 14 PPARg retinoid X receptor heterodimer 15 Increased free fatty acids and keto acids into the blood 16 Increased urea production Glucagon like peptide 1Function editGlucagon generally elevates the concentration of glucose in the blood by promoting gluconeogenesis and glycogenolysis 17 Glucagon also decreases fatty acid synthesis in adipose tissue and the liver as well as promoting lipolysis in these tissues which causes them to release fatty acids into circulation where they can be catabolised to generate energy in tissues such as skeletal muscle when required 18 Glucose is stored in the liver in the form of the polysaccharide glycogen which is a glucan a polymer made up of glucose molecules Liver cells hepatocytes have glucagon receptors When glucagon binds to the glucagon receptors the liver cells convert the glycogen into individual glucose molecules and release them into the bloodstream in a process known as glycogenolysis As these stores become depleted glucagon then encourages the liver and kidney to synthesize additional glucose by gluconeogenesis Glucagon turns off glycolysis in the liver causing glycolytic intermediates to be shuttled to gluconeogenesis Glucagon also regulates the rate of glucose production through lipolysis Glucagon induces lipolysis in humans under conditions of insulin suppression such as diabetes mellitus type 1 19 Glucagon production appears to be dependent on the central nervous system through pathways yet to be defined In invertebrate animals eyestalk removal has been reported to affect glucagon production Excising the eyestalk in young crayfish produces glucagon induced hyperglycemia 20 Mechanism of action edit nbsp Metabolic regulation of glycogen by glucagon Glucagon binds to the glucagon receptor a G protein coupled receptor located in the plasma membrane of the cell The conformation change in the receptor activates a G protein a heterotrimeric protein with as b and g subunits When the G protein interacts with the receptor it undergoes a conformational change that results in the replacement of the GDP molecule that was bound to the a subunit with a GTP molecule 21 This substitution results in the releasing of the a subunit from the b and g subunits The alpha subunit specifically activates the next enzyme in the cascade adenylate cyclase Adenylate cyclase manufactures cyclic adenosine monophosphate cyclic AMP or cAMP which activates protein kinase A cAMP dependent protein kinase This enzyme in turn activates phosphorylase kinase which then phosphorylates glycogen phosphorylase b PYG b converting it into the active form called phosphorylase a PYG a Phosphorylase a is the enzyme responsible for the release of glucose 1 phosphate from glycogen polymers An example of the pathway would be when glucagon binds to a transmembrane protein The transmembrane proteins interacts with Gɑb𝛾 Gas separates from Gb𝛾 and interacts with the transmembrane protein adenylyl cyclase Adenylyl cyclase catalyzes the conversion of ATP to cAMP cAMP binds to protein kinase A and the complex phosphorylates glycogen phosphorylase kinase 22 Phosphorylated glycogen phosphorylase kinase phosphorylates glycogen phosphorylase Phosphorylated glycogen phosphorylase clips glucose units from glycogen as glucose 1 phosphate Additionally the coordinated control of glycolysis and gluconeogenesis in the liver is adjusted by the phosphorylation state of the enzymes that catalyze the formation of a potent activator of glycolysis called fructose 2 6 bisphosphate 23 The enzyme protein kinase A PKA that was stimulated by the cascade initiated by glucagon will also phosphorylate a single serine residue of the bifunctional polypeptide chain containing both the enzymes fructose 2 6 bisphosphatase and phosphofructokinase 2 This covalent phosphorylation initiated by glucagon activates the former and inhibits the latter This regulates the reaction catalyzing fructose 2 6 bisphosphate a potent activator of phosphofructokinase 1 the enzyme that is the primary regulatory step of glycolysis 24 by slowing the rate of its formation thereby inhibiting the flux of the glycolysis pathway and allowing gluconeogenesis to predominate This process is reversible in the absence of glucagon and thus the presence of insulin Glucagon stimulation of PKA inactivates the glycolytic enzyme pyruvate kinase 25 inactivates glycogen synthase 26 and activates hormone sensitive lipase 27 which catabolizes glycerides into glycerol and free fatty acid s in hepatocytes Glucagon also inactivates acetyl CoA carboxylase which creates malonyl CoA from acetyl CoA through cAMP dependent and or cAMP independent kinases 28 Malonyl CoA is a byproduct of the Krebs cycle downstream of glycolysis and an allosteric inhibitor of Carnitine palmitoyltransferase I CPT1 a mitochondrial enzyme important for bringing fatty acids into the intermembrane space of the mitochondria for b oxidation 29 Glucagon decreases malonyl CoA through inhibition of acetyl CoA carboxylase and through reduced glycolysis through its aforementioned reduction in Fructose 2 6 bisphosphate Thus reduction in malonyl CoA is a common regulator for the increased fatty acid metabolism effects of glucagon Pathology editAbnormally elevated levels of glucagon may be caused by pancreatic tumors such as glucagonoma symptoms of which include necrolytic migratory erythema 30 reduced amino acids and hyperglycemia It may occur alone or in the context of multiple endocrine neoplasia type 1 31 Elevated glucagon is the main contributor to hyperglycemic ketoacidosis in undiagnosed or poorly treated type 1 diabetes As the beta cells cease to function insulin and pancreatic GABA are no longer present to suppress the freerunning output of glucagon As a result glucagon is released from the alpha cells at a maximum causing a rapid breakdown of glycogen to glucose and fast ketogenesis 32 It was found that a subset of adults with type 1 diabetes took 4 times longer on average to approach ketoacidosis when given somatostatin inhibits glucagon production with no insulin citation needed Inhibiting glucagon has been a popular idea of diabetes treatment however some have warned that doing so will give rise to brittle diabetes in patients with adequately stable blood glucose citation needed The absence of alpha cells and hence glucagon is thought to be one of the main influences in the extreme volatility of blood glucose in the setting of a total pancreatectomy History editIn the early 1920s several groups noted that pancreatic extracts injected into diabetic animals would result in a brief increase in blood sugar prior to the insulin driven decrease in blood sugar 6 In 1922 C Kimball and John R Murlin identified a component of pancreatic extracts responsible for this blood sugar increase terming it glucagon a portmanteau of glucose agonist 6 33 In the 1950s scientists at Eli Lilly isolated pure glucagon crystallized it and determined its amino acid sequence 6 34 35 This led to the development of the first radioimmunoassay for detecting glucagon described by Roger Unger s group in 1959 6 A more complete understanding of its role in physiology and disease was not established until the 1970s when a specific radioimmunoassay was developed 36 See also editCortisol Diabetes mellitus Glucagon like peptide 1 Glucagon like peptide 2 Insulin Islets of Langerhans Pancreas Proglucagon Tyrosine kinaseReferences edit Voet D Voet JG 2011 Biochemistry 4th ed New York Wiley Reece J Campbell N 2002 Biology San Francisco Benjamin Cummings ISBN 978 0 8053 6624 2 Orsay J 2014 Biology 1 Molecules Examkrackers Inc p 77 ISBN 978 1 893858 70 1 Jones BJ Tan T Bloom SR March 2012 Minireview Glucagon in stress and energy homeostasis Endocrinology 153 3 1049 54 doi 10 1210 en 2011 1979 PMC 3281544 PMID 22294753 Unger RH Orci L June 1981 Glucagon and the A cell physiology and pathophysiology first two parts The New England Journal of Medicine 304 25 1518 24 doi 10 1056 NEJM198106183042504 PMID 7015132 a b c d e f Muller TD Finan B Clemmensen C DiMarchi RD Tschop MH April 2017 The New Biology and Pharmacology of Glucagon Physiol Rev 97 2 721 766 doi 10 1152 physrev 00025 2016 PMID 28275047 Unger RH Cherrington AD January 2012 Glucagonocentric restructuring of diabetes a pathophysiologic and therapeutic makeover The Journal of Clinical Investigation 122 1 4 12 doi 10 1172 JCI60016 PMC 3248306 PMID 22214853 Holst JJ Holland W Gromada J Lee Y Unger RH Yan H Sloop KW Kieffer TJ Damond N Herrera PL April 2017 Insulin and Glucagon Partners for Life Endocrinology 158 4 696 701 doi 10 1210 en 2016 1748 PMC 6061217 PMID 28323959 a b Zhang XX Pan YH Huang YM Zhao HL May 2016 Neuroendocrine hormone amylin in diabetes World Journal of Diabetes 7 9 189 197 doi 10 4239 wjd v7 i9 189 PMC 4856891 PMID 27162583 Layden BT Durai V Lowe WL 2010 G Protein Coupled Receptors PANCREATIC Islets and DiAbetes Nature Education 3 9 13 Skoglund G Lundquist I Ahren B November 1987 Alpha 1 and alpha 2 adrenoceptor activation increases plasma glucagon levels in the mouse European Journal of Pharmacology 143 1 83 8 doi 10 1016 0014 2999 87 90737 0 PMID 2891547 Honey RN Weir GC October 1980 Acetylcholine stimulates insulin glucagon and somatostatin release in the perfused chicken pancreas Endocrinology 107 4 1065 8 doi 10 1210 endo 107 4 1065 PMID 6105951 REHFELD JENS February 1978 The effect of gastrin on basal and aminoacid stimulated insulin and glucagon secretion in man European Journal of Clinical Investigation 8 1 5 9 doi 10 1111 j 1365 2362 1978 tb00800 x PMID 417933 S2CID 38154468 Xu E Kumar M Zhang Y Ju W Obata T Zhang N Liu S Wendt A Deng S Ebina Y Wheeler MB Braun M Wang Q January 2006 Intra islet insulin suppresses glucagon release via GABA GABAA receptor system Cell Metabolism 3 1 47 58 doi 10 1016 j cmet 2005 11 015 PMID 16399504 Kratzner R Frohlich F Lepler K Schroder M Roher K Dickel C Tzvetkov MV Quentin T Oetjen E Knepel W February 2008 A peroxisome proliferator activated receptor gamma retinoid X receptor heterodimer physically interacts with the transcriptional activator PAX6 to inhibit glucagon gene transcription Molecular Pharmacology 73 2 509 17 doi 10 1124 mol 107 035568 PMID 17962386 S2CID 10108970 Johnson LR 2003 Essential Medical Physiology Academic Press pp 643 ISBN 978 0 12 387584 6 Voet D Voet JG 2011 Biochemistry 4th ed New York Wiley Habegger KM Heppner KM Geary N Bartness TJ DiMarchi R Tschop MH December 2010 The metabolic actions of glucagon revisited Nature Reviews Endocrinology 6 12 689 697 doi 10 1038 nrendo 2010 187 PMC 3563428 PMID 20957001 Liljenquist JE Bomboy JD Lewis SB Sinclair Smith BC Felts PW Lacy WW Crofford OB Liddle GW January 1974 Effects of glucagon on lipolysis and ketogenesis in normal and diabetic men The Journal of Clinical Investigation 53 1 190 7 doi 10 1172 JCI107537 PMC 301453 PMID 4808635 Leinen RL Giannini AJ 1983 Effect of eyestalk removal on glucagon induced hyperglycemia in crayfish Society for Neuroscience Abstracts 9 604 Glucagon Signaling Pathway News Medical net 2018 03 01 Retrieved 2021 03 30 Yu Q Shuai H Ahooghalandari P Gylfe E Tengholm A July 2019 Glucose controls glucagon secretion by directly modulating cAMP in alpha cells Diabetologia 62 7 1212 1224 doi 10 1007 s00125 019 4857 6 PMC 6560012 PMID 30953108 Hue L Rider MH July 1987 Role of fructose 2 6 bisphosphate in the control of glycolysis in mammalian tissues The Biochemical Journal 245 2 313 24 doi 10 1042 bj2450313 PMC 1148124 PMID 2822019 Claus TH El Maghrabi MR Regen DM Stewart HB McGrane M Kountz PD Nyfeler F Pilkis J Pilkis SJ 1984 The Role of Fructose 2 6 Bisphosphate in the Regulation of Carbohydrate Metabolism Current Topics in Cellular Regulation Vol 23 pp 57 86 doi 10 1016 b978 0 12 152823 2 50006 4 ISBN 9780121528232 PMID 6327193 Feliu JE Hue L Hers HG August 1976 Hormonal control of pyruvate kinase activity and of gluconeogenesis in isolated hepatocytes Proceedings of the National Academy of Sciences of the United States of America 73 8 2762 6 Bibcode 1976PNAS 73 2762F doi 10 1073 pnas 73 8 2762 PMC 430732 PMID 183209 Jiang G Zhang BB April 2003 Glucagon and regulation of glucose metabolism Am J Physiol Endocrinol Metab 284 4 E671 8 doi 10 1152 ajpendo 00492 2002 PMID 12626323 Hayashi Y January 2021 Glucagon regulates lipolysis and fatty acid oxidation through inositol triphosphate receptor 1 in the liver Diabetes Investig 12 1 32 34 doi 10 1111 jdi 13315 PMC 7779274 PMID 32506830 Swenson TL Porter JW Mar 25 1985 Mechanism of glucagon inhibition of liver acetyl CoA carboxylase Interrelationship of the effects of phosphorylation polymer protomer transition and citrate on enzyme activity The Journal of Biological Chemistry 2460 6 3791 3797 doi 10 1016 S0021 9258 19 83693 1 PMID 2857722 Wang Y Yu W Li S Guo D He J Wang Y March 11 2022 Acetyl CoA Carboxylases and Diseases Frontiers in Oncology 12 doi 10 3389 fonc 2022 836058 PMC 8963101 PMID 35359351 John AM Schwartz RA December 2016 Glucagonoma syndrome a review and update on treatment Journal of the European Academy of Dermatology and Venereology 30 12 2016 2022 doi 10 1111 jdv 13752 PMID 27422767 S2CID 1228654 Oberg K December 2010 Pancreatic endocrine tumors Seminars in Oncology 37 6 594 618 doi 10 1053 j seminoncol 2010 10 014 PMID 21167379 Fasanmade OA Odeniyi IA Ogbera AO June 2008 Diabetic ketoacidosis diagnosis and management African Journal of Medicine and Medical Sciences 37 2 99 105 PMID 18939392 Kimball C Murlin J 1923 Aqueous extracts of pancreas III Some precipitation reactions of insulin J Biol Chem 58 1 337 348 doi 10 1016 S0021 9258 18 85474 6 Staub A Sinn L Behrens OK June 1953 Purification and crystallization of hyperglycemic glycogenolytic factor HGF Science 117 3049 628 9 Bibcode 1953Sci 117 628S doi 10 1126 science 117 3049 628 PMID 13056638 Bromer W Winn L Behrens O 1957 The amino acid sequence of glucagon V Location of amide groups acid degradation studies and summary of sequential evidence J Am Chem Soc 79 11 2807 2810 doi 10 1021 ja01568a038 Lundqvist Gudmar Edwards John Wide Leif January 1976 A Solid Phase Radioimmunoassay for Pancreatic Glucagon Upsala Journal of Medical Sciences 81 2 65 69 doi 10 3109 03009737609179024 ISSN 0300 9734 PMID 785743 External links editListen to this article 10 minutes source source nbsp This audio file was created from a revision of this article dated 16 August 2019 2019 08 16 and does not reflect subsequent edits Audio help More spoken articles PDBe KB provides an overview of all the structure information available in the PDB for Human Glucagon Retrieved from https en wikipedia org w index php title Glucagon amp oldid 1186282197, wikipedia, wiki, book, books, library,

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