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Gluconeogenesis

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<StructureSection load='2y3i' size='350' side='right' scene='' caption='Human phosphoglycerate kinase complex with phosphoglyceric acid, ADP (stick model) AlF4-, Cl- and Mg+2 ions (green) (PDB code [[2y3i]])'>
<StructureSection load='2y3i' size='350' side='right' scene='' caption='Human phosphoglycerate kinase complex with phosphoglyceric acid, ADP (stick model) AlF4-, Cl- and Mg+2 ions (green) (PDB code [[2y3i]])'>
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'''Under development!'''
 
Gluconeogenesis ([https://en.wikipedia.org/wiki/Gluconeogenesis]) is a metabolic pathway that results in the generation of glucose from certain non-carbohydrate carbon substrates. In humans the main gluconeogenic precursors are lactate, <scene name='92/925544/Cv/1'>glycerol</scene> (which is a part of the triglyceride molecule), alanine and glutamine. Other glucogenic amino acids and all [[Citric Acid Cycle]] intermediates (through conversion to oxaloacetate) can also function as substrates for gluconeogenesis. See also [[Cori cycle]] and [[Glyoxylate cycle]].
Gluconeogenesis ([https://en.wikipedia.org/wiki/Gluconeogenesis]) is a metabolic pathway that results in the generation of glucose from certain non-carbohydrate carbon substrates. In humans the main gluconeogenic precursors are lactate, <scene name='92/925544/Cv/1'>glycerol</scene> (which is a part of the triglyceride molecule), alanine and glutamine. Other glucogenic amino acids and all [[Citric Acid Cycle]] intermediates (through conversion to oxaloacetate) can also function as substrates for gluconeogenesis. See also [[Cori cycle]] and [[Glyoxylate cycle]].

Revision as of 14:43, 19 February 2023

Human phosphoglycerate kinase complex with phosphoglyceric acid, ADP (stick model) AlF4-, Cl- and Mg+2 ions (green) (PDB code 2y3i)

Drag the structure with the mouse to rotate

References

  1. Dunten P, Belunis C, Crowther R, Hollfelder K, Kammlott U, Levin W, Michel H, Ramsey GB, Swain A, Weber D, Wertheimer SJ. Crystal structure of human cytosolic phosphoenolpyruvate carboxykinase reveals a new GTP-binding site. J Mol Biol. 2002 Feb 15;316(2):257-64. PMID:11851336 doi:http://dx.doi.org/10.1006/jmbi.2001.5364

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