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Metabolic pathway

February 16, 2024

In biochemistry, a metabolic pathway is a linked series of chemical reactions occurring within a cell. The reactants, products, and intermediates of an enzymatic reaction are known as metabolites, which are modified by a sequence of chemical reactions catalyzed by enzymes.[1]: 26  In most cases of a metabolic pathway, the product of one enzyme acts as the substrate for the next. However, side products are considered waste and removed from the cell.[2] These enzymes often require dietary minerals, vitamins, and other cofactors to function.[citation needed]

Different metabolic pathways function in the position within a eukaryotic cell and the significance of the pathway in the given compartment of the cell.[3] For instance, the electron transport chain and oxidative phosphorylation all take place in the mitochondrial membrane.[4]: 73, 74 & 109  In contrast, glycolysis, pentose phosphate pathway, and fatty acid biosynthesis all occur in the cytosol of a cell.[5]: 441–442 

There are two types of metabolic pathways that are characterized by their ability to either synthesize molecules with the utilization of energy (anabolic pathway), or break down complex molecules and release energy in the process (catabolic pathway).[6]

The two pathways complement each other in that the energy released from one is used up by the other. The degradative process of a catabolic pathway provides the energy required to conduct the biosynthesis of an anabolic pathway.[6] In addition to the two distinct metabolic pathways is the amphibolic pathway, which can be either catabolic or anabolic based on the need for or the availability of energy.[7]

Pathways are required for the maintenance of homeostasis within an organism and the flux of metabolites through a pathway is regulated depending on the needs of the cell and the availability of the substrate. The end product of a pathway may be used immediately, initiate another metabolic pathway or be stored for later use. The metabolism of a cell consists of an elaborate network of interconnected pathways that enable the synthesis and breakdown of molecules (anabolism and catabolism).

Overview edit

 
Net reactions of common metabolic pathways

Each metabolic pathway consists of a series of biochemical reactions that are connected by their intermediates: the products of one reaction are the substrates for subsequent reactions, and so on. Metabolic pathways are often considered to flow in one direction. Although all chemical reactions are technically reversible, conditions in the cell are often such that it is thermodynamically more favorable for flux to proceed in one direction of a reaction.[8] For example, one pathway may be responsible for the synthesis of a particular amino acid, but the breakdown of that amino acid may occur via a separate and distinct pathway. One example of an exception to this "rule" is the metabolism of glucose. Glycolysis results in the breakdown of glucose, but several reactions in the glycolysis pathway are reversible and participate in the re-synthesis of glucose (gluconeogenesis).[citation needed]

  • Glycolysis was the first metabolic pathway discovered:
  1. As glucose enters a cell, it is immediately phosphorylated by ATP to glucose 6-phosphate in the irreversible first step.
  2. In times of excess lipid or protein energy sources, certain reactions in the glycolysis pathway may run in reverse to produce glucose 6-phosphate, which is then used for storage as glycogen or starch.
  • Metabolic pathways are often regulated by feedback inhibition.
  • Some metabolic pathways flow in a 'cycle' wherein each component of the cycle is a substrate for the subsequent reaction in the cycle, such as in the Krebs Cycle (see below).
  • Anabolic and catabolic pathways in eukaryotes often occur independently of each other, separated either physically by compartmentalization within organelles or separated biochemically by the requirement of different enzymes and co-factors.

Major metabolic pathways edit

For additional infographics of major metabolic pathways, see § External links.
 



MEP
MVA
 
Major metabolic pathways in metro-style map. Click any text (name of pathway or metabolites) to link to the corresponding article.
Single lines: pathways common to most lifeforms. Double lines: pathways not in humans (occurs in e.g. plants, fungi, prokaryotes).   Orange nodes: carbohydrate metabolism.   Violet nodes: photosynthesis.   Red nodes: cellular respiration.   Pink nodes: cell signaling.   Blue nodes: amino acid metabolism.   Grey nodes: vitamin and cofactor metabolism.   Brown nodes: nucleotide and protein metabolism.   Green nodes: lipid metabolism.

Catabolic pathway (catabolism) edit

A catabolic pathway is a series of reactions that bring about a net release of energy in the form of a high energy phosphate bond formed with the energy carriers adenosine diphosphate (ADP) and guanosine diphosphate (GDP) to produce adenosine triphosphate (ATP) and guanosine triphosphate (GTP), respectively.[4]: 91–93  The net reaction is, therefore, thermodynamically favorable, for it results in a lower free energy for the final products.[9]: 578–579  A catabolic pathway is an exergonic system that produces chemical energy in the form of ATP, GTP, NADH, NADPH, FADH2, etc. from energy containing sources such as carbohydrates, fats, and proteins. The end products are often carbon dioxide, water, and ammonia. Coupled with an endergonic reaction of anabolism, the cell can synthesize new macromolecules using the original precursors of the anabolic pathway.[10] An example of a coupled reaction is the phosphorylation of fructose-6-phosphate to form the intermediate fructose-1,6-bisphosphate by the enzyme phosphofructokinase accompanied by the hydrolysis of ATP in the pathway of glycolysis. The resulting chemical reaction within the metabolic pathway is highly thermodynamically favorable and, as a result, irreversible in the cell.

 

Cellular respiration edit

Main article: Cellular respiration

A core set of energy-producing catabolic pathways occur within all living organisms in some form. These pathways transfer the energy released by breakdown of nutrients into ATP and other small molecules used for energy (e.g. GTP, NADPH, FADH2). All cells can perform anaerobic respiration by glycolysis. Additionally, most organisms can perform more efficient aerobic respiration through the citric acid cycle and oxidative phosphorylation. Additionally plants, algae and cyanobacteria are able to use sunlight to anabolically synthesize compounds from non-living matter by photosynthesis.

 
Gluconeogenesis Mechanism

Anabolic pathway (anabolism) edit

In contrast to catabolic pathways, anabolic pathways require an energy input to construct macromolecules such as polypeptides, nucleic acids, proteins, polysaccharides, and lipids. The isolated reaction of anabolism is unfavorable in a cell due to a positive Gibbs Free Energy (+ΔG). Thus, an input of chemical energy through a coupling with an exergonic reaction is necessary.[1]: 25–27  The coupled reaction of the catabolic pathway affects the thermodynamics of the reaction by lowering the overall activation energy of an anabolic pathway and allowing the reaction to take place.[1]: 25  Otherwise, an endergonic reaction is non-spontaneous.

An anabolic pathway is a biosynthetic pathway, meaning that it combines smaller molecules to form larger and more complex ones.[9]: 570  An example is the reversed pathway of glycolysis, otherwise known as gluconeogenesis, which occurs in the liver and sometimes in the kidney to maintain proper glucose concentration in the blood and supply the brain and muscle tissues with adequate amount of glucose. Although gluconeogenesis is similar to the reverse pathway of glycolysis, it contains four distinct enzymes(pyruvate carboxylase, phosphoenolpyruvate carboxykinase, fructose 1,6-bisphosphatase, glucose 6-phosphatase) from glycolysis that allow the pathway to occur spontaneously.[11]

Amphibolic pathway edit

 
Amphibolic Properties of the Citric Acid Cycle

An amphibolic pathway is one that can be either catabolic or anabolic based on the availability of or the need for energy.[9]: 570  The currency of energy in a biological cell is adenosine triphosphate (ATP), which stores its energy in the phosphoanhydride bonds. The energy is utilized to conduct biosynthesis, facilitate movement, and regulate active transport inside of the cell.[9]: 571  Examples of amphibolic pathways are the citric acid cycle and the glyoxylate cycle. These sets of chemical reactions contain both energy producing and utilizing pathways.[5]: 572  To the right is an illustration of the amphibolic properties of the TCA cycle.

The glyoxylate shunt pathway is an alternative to the tricarboxylic acid (TCA) cycle, for it redirects the pathway of TCA to prevent full oxidation of carbon compounds, and to preserve high energy carbon sources as future energy sources. This pathway occurs only in plants and bacteria and transpires in the absence of glucose molecules.[12]

Regulation edit

The flux of the entire pathway is regulated by the rate-determining steps.[1]: 577–578  These are the slowest steps in a network of reactions. The rate-limiting step occurs near the beginning of the pathway and is regulated by feedback inhibition, which ultimately controls the overall rate of the pathway.[13] The metabolic pathway in the cell is regulated by covalent or non-covalent modifications. A covalent modification involves an addition or removal of a chemical bond, whereas a non-covalent modification (also known as allosteric regulation) is the binding of the regulator to the enzyme via hydrogen bonds, electrostatic interactions, and Van Der Waals forces.[14]

The rate of turnover in a metabolic pathway, also known as the metabolic flux, is regulated based on the stoichiometric reaction model, the utilization rate of metabolites, and the translocation pace of molecules across the lipid bilayer.[15] The regulation methods are based on experiments involving 13C-labeling, which is then analyzed by Nuclear Magnetic Resonance (NMR) or gas chromatography-mass spectrometry (GC-MS)-derived mass compositions. The aforementioned techniques synthesize a statistical interpretation of mass distribution in proteinogenic amino acids to the catalytic activities of enzymes in a cell.[15]: 178 

Clinical applications in targeting metabolic pathways edit

Targeting Oxidative Phosphorylation edit

Metabolic pathways can be targeted for clinically therapeutic uses. Within the mitochondrial metabolic network, for instance, there are various pathways that can be targeted by compounds to prevent cancer cell proliferation.[16] One such pathway is oxidative phosphorylation (OXPHOS) within the electron transport chain (ETC). Various inhibitors can downregulate the electrochemical reactions that take place at Complex I, II, III, and IV, thereby preventing the formation of an electrochemical gradient and downregulating the movement of electrons through the ETC. The substrate-level phosphorylation that occurs at ATP synthase can also be directly inhibited, preventing the formation of ATP that is necessary to supply energy for cancer cell proliferation.[17] Some of these inhibitors, such as lonidamine and atovaquone,[16] which inhibit Complex II and Complex III, respectively, are currently undergoing clinical trials for FDA-approval. Other non-FDA-approved inhibitors have still shown experimental success in vitro.

Targeting Heme edit

Heme, an important prosthetic group present in Complexes I, II, and IV can also be targeted, since heme biosynthesis and uptake have been correlated with increased cancer progression.[18] Various molecules can inhibit heme via different mechanisms. For instance, succinylacetone has been shown to decrease heme concentrations by inhibiting δ-aminolevulinic acid in murine erythroleukemia cells.[19] The primary structure of heme-sequestering peptides, such as HSP1 and HSP2, can be modified to downregulate heme concentrations and reduce proliferation of non-small lung cancer cells.[20]

Targeting the Tricarboxylic acid cycle and Glutaminolysis edit

The tricarboxylic acid cycle (TCA) and glutaminolysis can also be targeted for cancer treatment, since they are essential for the survival and proliferation of cancer cells. Ivosidenib and Enasidenib, two FDA-approved cancer treatments, can arrest the TCA cycle of cancer cells by inhibiting isocitrate dehydrogenase-1 (IDH1) and isocitrate dehydrogenase-2 (IDH2), respectively.[16] Ivosidenib is specific to acute myeloid leukemia (AML) and cholangiocarcinoma, whereas Enasidenib is specific to just acute myeloid leukemia (AML).

In a clinical trial consisting of 185 adult patients with cholangiocarcinoma and an IDH-1 mutation, there was a statistically significant improvement (p<0.0001; HR: 0.37) in patients randomized to Ivosidenib. Still, some of the adverse side effects in these patients included fatigue, nausea, diarrhea, decreased appetite, ascites, and anemia.[21] In a clinical trial consisting of 199 adult patients with AML and an IDH2 mutation, 23% of patients experienced complete response (CR) or complete response with partial hematologic recovery (CRh) lasting a median of 8.2 months while on Enasidenib. Of the 157 patients who required transfusion at the beginning of the trial, 34% no longer required transfusions during the 56-day time period on Enasidenib. Of the 42% of patients who did not require transfusions at the beginning of the trial, 76% still did not require a transfusion by the end of the trial. Side effects of Enasidenib included nausea, diarrhea, elevated bilirubin and most notably, differentiation syndrome.[22]

Glutaminase (GLS), the enzyme responsible for converting glutamine to glutamate via hydrolytic deamidation during the first reaction of glutaminolysis, can also be targeted. In recent years, many small molecules, such as azaserine, acivicin, and CB-839 have been shown to inhibit glutaminase, thus reducing cancer cell viability and inducing apoptosis in cancer cells.[23] Due to its effective antitumor ability in several cancer types such as ovarian, breast and lung cancers, CB-839 is the only GLS inhibitor currently undergoing clinical studies for FDA-approval.

Genetic engineering of metabolic pathways edit

Many metabolic pathways are of commercial interest. For instance, the production of many antibiotics or other drugs requires complex pathways. The pathways to produce such compounds can be transplanted into microbes or other more suitable organism for production purposes. For example, the world's supply of the anti-cancer drug vinblastine is produced by relatively ineffient extraction and purification of the precursors vindoline and catharanthine from the plant Catharanthus roseus, which are then chemically converted into vinblastine. The biosynthetic pathway to produce vinblastine, including 30 enzymatic steps, has been transferred into yeast cells which is a convenient system to grow in large amounts. With these genetic modifications yeast can use its own metabolites geranyl pyrophosphate and tryptophan to produce the precursors of catharanthine and vindoline. This process required 56 genetic edits, including expression of 34 heterologous genes from plants in yeast cells.[24]

See also edit

References edit

  1. ^ a b c d Nelson DL, Cox MM (2008). Lehninger principles of biochemistry (5th ed.). New York: W.H. Freeman. ISBN 978-0-7167-7108-1.
  2. ^ Alison S, Papachristodoulou DK, Despo K, Elliott WH, Elliott DC (2014). Biochemistry and molecular biology (Fifth ed.). Oxford. ISBN 978-0-19-960949-9. OCLC 862091499.{{cite book}}: CS1 maint: location missing publisher (link)
  3. ^ Nicholson DE (March 1971). An Introduction to Metabolic Pathways by S. DAGLEY (Vol. 59, No. 2 ed.). Sigma Xi, The Scientific Research Society. p. 266.
  4. ^ a b Harvey RA (2011). Biochemistry (5th ed.). Baltimore, MD: Wolters Kluwer. ISBN 978-1-60831-412-6.
  5. ^ a b Voet D, Voet JD, Pratt CW (2013). Fundamentals of Biochemistry: Life at the Molecular Level (4th ed.). Hoboken, NJ: Wiley. ISBN 978-0470-54784-7.
  6. ^ a b Reece JB, Campbell NA (2011). Campbell Biology (9th ed.). Boston: Benjamin Cummings / Pearson. pp. 143. ISBN 978-0-321-55823-7.
  7. ^ Berg JM, Tymoczko JL, Stryer L, Gatto GJ (2012). Biochemistry (7th ed.). New York: W.H. Freeman. p. 429. ISBN 978-1-4292-2936-4.
  8. ^ Cornish-Bowden A, Cárdenas M (2000). "Irreversible reactions in metabolic simulations: how reversible is irreversible?" (PDF). Animating the Cellular Map: 65–71.
  9. ^ a b c d Berg JM, Tymoczko JL, Stryer L (2002). Biochemistry (5th ed.). New York, NY: W. H. Freeman. ISBN 978-0-7167-3051-4.
  10. ^ Raven PH, Evert RF, Eichhorn SE (2011). Biology of plants (8th ed.). New York, NY: Freeman. pp. 100–106. ISBN 978-1-4292-1961-7.
  11. ^ Berg JM, Tymoczko JL, Stryer L, Gatto GJ (2012). Biochemistry (7th ed.). New York: W.H. Freeman. pp. 480–482. ISBN 978-1-4292-2936-4.
  12. ^ Pray L, Relman DA, Choffnes ER, eds. (2011). The science and applications of synthetic and systems biology workshop summary. Washington, D.C.: National Academies Press. p. 135. ISBN 978-0-309-21939-6.
  13. ^ Hill SA, Ratcliffe RG (1999). Kruger NJ (ed.). Regulation of primary metabolic pathways in plants : [proceedings of an international conference held on 9 - 11 January 1997 at St Hugh's College, Oxford under the auspices of the Phytochemical Society of Europe]. Dordrecht [u.a.]: Kluwer. p. 258. ISBN 978-0-7923-5494-9.
  14. ^ White D (1995). The physiology and biochemistry of prokaryotes. New York [u.a.]: Oxford Univ. Press. p. 133. ISBN 978-0-19-508439-9.
  15. ^ a b Weckwerth W, ed. (2006). Metabolomics methods and protocols. Totowa, N.J.: Humana Press. p. 177. ISBN 978-1-59745-244-1.
  16. ^ a b c Frattaruolo L, Brindisi M, Curcio R, Marra F, Dolce V, Cappello AR (August 2020). "Targeting the Mitochondrial Metabolic Network: A Promising Strategy in Cancer Treatment". International Journal of Molecular Sciences. 21 (17): 2–11. doi:10.3390/ijms21176014. PMC 7503725. PMID 32825551.
  17. ^ Yadav N, Kumar S, Marlowe T, Chaudhary AK, Kumar R, Wang J, et al. (November 2015). "Oxidative phosphorylation-dependent regulation of cancer cell apoptosis in response to anticancer agents". Cell Death & Disease. 6 (11): e1969. doi:10.1038/cddis.2015.305. PMC 4670921. PMID 26539916.
  18. ^ Hooda J, Cadinu D, Alam MM, Shah A, Cao TM, Sullivan LA, et al. (2013). "Enhanced heme function and mitochondrial respiration promote the progression of lung cancer cells". PLOS ONE. 8 (5): e63402. Bibcode:2013PLoSO...863402H. doi:10.1371/journal.pone.0063402. PMC 3660535. PMID 23704904.
  19. ^ Ebert PS, Hess RA, Frykholm BC, Tschudy DP (June 1979). "Succinylacetone, a potent inhibitor of heme biosynthesis: effect on cell growth, heme content and delta-aminolevulinic acid dehydratase activity of malignant murine erythroleukemia cells". Biochemical and Biophysical Research Communications. 88 (4): 1382–1390. doi:10.1016/0006-291x(79)91133-1. PMID 289386.
  20. ^ Sohoni S, Ghosh P, Wang T, Kalainayakan SP, Vidal C, Dey S, et al. (May 2019). "Elevated Heme Synthesis and Uptake Underpin Intensified Oxidative Metabolism and Tumorigenic Functions in Non-Small Cell Lung Cancer Cells". Cancer Research. 79 (10): 2511–2525. doi:10.1158/0008-5472.CAN-18-2156. PMID 30902795. S2CID 85456667.
  21. ^ "FDA approves Ivosidenib for advanced or metastatic cholangiocarcinoma". U.S. Food & Drug Administration. 26 August 2021.
  22. ^ "FDA granted regular approval to enasidenib for the treatment of relapsed or refractory AML". U.S. Food & Drug Administration. 9 February 2019.
  23. ^ Matés JM, Di Paola FJ, Campos-Sandoval JA, Mazurek S, Márquez J (February 2020). "Therapeutic targeting of glutaminolysis as an essential strategy to combat cancer". Seminars in Cell & Developmental Biology. 98: 34–43. doi:10.1016/j.semcdb.2019.05.012. PMID 31100352. S2CID 157067127.
  24. ^ Zhang J, Hansen LG, Gudich O, Viehrig K, Lassen LM, Schrübbers L, et al. (September 2022). "A microbial supply chain for production of the anti-cancer drug vinblastine". Nature. 609 (7926): 341–347. Bibcode:2022Natur.609..341Z. doi:10.1038/s41586-022-05157-3. PMC 9452304. PMID 36045295.

External links edit

 
Wikimedia Commons has media related to Metabolic pathways.
  • Full map of metabolic pathways
  • Biochemical pathways, Gerhard Michal
  • Overview Map from BRENDA
  • BioCyc: Metabolic network models for thousands of sequenced organisms
  • KEGG: Kyoto Encyclopedia of Genes and Genomes
  • Reactome, a database of reactions, pathways and biological processes
  • MetaCyc: A database of experimentally elucidated metabolic pathways (2,200+ pathways from more than 2,500 organisms).
  • MetaboMAPS: A platform for pathway sharing and data visualization on metabolic pathways
  • DAVID: Visualize genes on pathway maps
  • Wikipathways: pathways for the people
  • ConsensusPathDB
  • metpath: Integrated interactive metabolic chart
Metabolic pathway diagram
  All pathway labels on this image are links, simply click to access the article.
A high resolution labeled version of this image is available here.  

February 16, 2024
metabolic, pathway, biochemistry, metabolic, pathway, linked, series, chemical, reactions, occurring, within, cell, reactants, products, intermediates, enzymatic, reaction, known, metabolites, which, modified, sequence, chemical, reactions, catalyzed, enzymes,. In biochemistry a metabolic pathway is a linked series of chemical reactions occurring within a cell The reactants products and intermediates of an enzymatic reaction are known as metabolites which are modified by a sequence of chemical reactions catalyzed by enzymes 1 26 In most cases of a metabolic pathway the product of one enzyme acts as the substrate for the next However side products are considered waste and removed from the cell 2 These enzymes often require dietary minerals vitamins and other cofactors to function citation needed Different metabolic pathways function in the position within a eukaryotic cell and the significance of the pathway in the given compartment of the cell 3 For instance the electron transport chain and oxidative phosphorylation all take place in the mitochondrial membrane 4 73 74 amp 109 In contrast glycolysis pentose phosphate pathway and fatty acid biosynthesis all occur in the cytosol of a cell 5 441 442 There are two types of metabolic pathways that are characterized by their ability to either synthesize molecules with the utilization of energy anabolic pathway or break down complex molecules and release energy in the process catabolic pathway 6 The two pathways complement each other in that the energy released from one is used up by the other The degradative process of a catabolic pathway provides the energy required to conduct the biosynthesis of an anabolic pathway 6 In addition to the two distinct metabolic pathways is the amphibolic pathway which can be either catabolic or anabolic based on the need for or the availability of energy 7 Pathways are required for the maintenance of homeostasis within an organism and the flux of metabolites through a pathway is regulated depending on the needs of the cell and the availability of the substrate The end product of a pathway may be used immediately initiate another metabolic pathway or be stored for later use The metabolism of a cell consists of an elaborate network of interconnected pathways that enable the synthesis and breakdown of molecules anabolism and catabolism Contents 1 Overview 2 Major metabolic pathways 2 1 Catabolic pathway catabolism 2 1 1 Cellular respiration 2 2 Anabolic pathway anabolism 2 3 Amphibolic pathway 3 Regulation 4 Clinical applications in targeting metabolic pathways 4 1 Targeting Oxidative Phosphorylation 4 2 Targeting Heme 4 3 Targeting the Tricarboxylic acid cycle and Glutaminolysis 5 Genetic engineering of metabolic pathways 6 See also 7 References 8 External linksOverview edit nbsp Net reactions of common metabolic pathwaysEach metabolic pathway consists of a series of biochemical reactions that are connected by their intermediates the products of one reaction are the substrates for subsequent reactions and so on Metabolic pathways are often considered to flow in one direction Although all chemical reactions are technically reversible conditions in the cell are often such that it is thermodynamically more favorable for flux to proceed in one direction of a reaction 8 For example one pathway may be responsible for the synthesis of a particular amino acid but the breakdown of that amino acid may occur via a separate and distinct pathway One example of an exception to this rule is the metabolism of glucose Glycolysis results in the breakdown of glucose but several reactions in the glycolysis pathway are reversible and participate in the re synthesis of glucose gluconeogenesis citation needed Glycolysis was the first metabolic pathway discovered As glucose enters a cell it is immediately phosphorylated by ATP to glucose 6 phosphate in the irreversible first step In times of excess lipid or protein energy sources certain reactions in the glycolysis pathway may run in reverse to produce glucose 6 phosphate which is then used for storage as glycogen or starch Metabolic pathways are often regulated by feedback inhibition Some metabolic pathways flow in a cycle wherein each component of the cycle is a substrate for the subsequent reaction in the cycle such as in the Krebs Cycle see below Anabolic and catabolic pathways in eukaryotes often occur independently of each other separated either physically by compartmentalization within organelles or separated biochemically by the requirement of different enzymes and co factors Major metabolic pathways editFor additional infographics of major metabolic pathways see External links nbsp Carbonfixation Photo respiration Pentosephosphatepathway Citricacid cycle Glyoxylatecycle Ureacycle Fattyacidsynthesis Fattyacidelongation Betaoxidation Peroxisomal betaoxidation Glyco genolysis Glyco genesis Glyco lysis Gluconeo genesis Pyruvatedecarb oxylation Fermentation Keto lysis Keto genesis feeders togluconeo genesis Direct C4 CAMcarbon intake Light reaction Oxidativephosphorylation Amino aciddeamination Citrateshuttle Lipogenesis Lipolysis Steroidogenesis MVA pathway MEP pathway Shikimatepathway Transcription amp replication Translation Proteolysis Glycosyl ation Sugaracids Double multiplesugars amp glycans Simplesugars Inositol P Amino sugars amp sialic acids Nucleotide sugars Hexose P Triose P Glycerol P glycerates Pentose P Tetrose P Propionyl CoA Succinate Acetyl CoA Pentose P P glycerates Glyoxylate Photosystems Pyruvate Lactate Acetyl CoA Citrate Oxalo acetate Malate Succinyl CoA a Keto glutarate Ketonebodies Respiratorychain Serine group Alanine Branched chainamino acids Aspartategroup Homoserinegroup amp lysine Glutamategroup amp proline Arginine Creatine amp polyamines Ketogenic amp glucogenicamino acids Amino acids Shikimate Aromatic aminoacids amp histidine Ascorbate vitamin C d ALA Bilepigments Hemes Cobalamins vitamin B12 Variousvitamin Bs Calciferols vitamin D Retinoids vitamin A Quinones vitamin K amp tocopherols vitamin E Cofactors Vitamins amp minerals Antioxidants PRPP Nucleotides Nucleicacids Proteins Glycoproteins amp proteoglycans Chlorophylls MEP MVA Acetyl CoA Polyketides Terpenoidbackbones Terpenoids amp carotenoids vitamin A Cholesterol Bile acids Glycero phospholipids Glycerolipids Acyl CoA Fattyacids Glyco sphingolipids Sphingolipids Waxes Polyunsaturatedfatty acids Neurotransmitters amp thyroid hormones Steroids Endo cannabinoids Eicosanoids nbsp Major metabolic pathways in metro style map Click any text name of pathway or metabolites to link to the corresponding article Single lines pathways common to most lifeforms Double lines pathways not in humans occurs in e g plants fungi prokaryotes nbsp Orange nodes carbohydrate metabolism nbsp Violet nodes photosynthesis nbsp Red nodes cellular respiration nbsp Pink nodes cell signaling nbsp Blue nodes amino acid metabolism nbsp Grey nodes vitamin and cofactor metabolism nbsp Brown nodes nucleotide and protein metabolism nbsp Green nodes lipid metabolism Catabolic pathway catabolism edit A catabolic pathway is a series of reactions that bring about a net release of energy in the form of a high energy phosphate bond formed with the energy carriers adenosine diphosphate ADP and guanosine diphosphate GDP to produce adenosine triphosphate ATP and guanosine triphosphate GTP respectively 4 91 93 The net reaction is therefore thermodynamically favorable for it results in a lower free energy for the final products 9 578 579 A catabolic pathway is an exergonic system that produces chemical energy in the form of ATP GTP NADH NADPH FADH2 etc from energy containing sources such as carbohydrates fats and proteins The end products are often carbon dioxide water and ammonia Coupled with an endergonic reaction of anabolism the cell can synthesize new macromolecules using the original precursors of the anabolic pathway 10 An example of a coupled reaction is the phosphorylation of fructose 6 phosphate to form the intermediate fructose 1 6 bisphosphate by the enzyme phosphofructokinase accompanied by the hydrolysis of ATP in the pathway of glycolysis The resulting chemical reaction within the metabolic pathway is highly thermodynamically favorable and as a result irreversible in the cell Fructose 6 Phosphate ATP Fructose 1 6 Bisphosphate ADP displaystyle ce Fructose 6 Phosphate ATP gt Fructose 1 6 Bisphosphate ADP nbsp Cellular respiration edit Main article Cellular respiration A core set of energy producing catabolic pathways occur within all living organisms in some form These pathways transfer the energy released by breakdown of nutrients into ATP and other small molecules used for energy e g GTP NADPH FADH2 All cells can perform anaerobic respiration by glycolysis Additionally most organisms can perform more efficient aerobic respiration through the citric acid cycle and oxidative phosphorylation Additionally plants algae and cyanobacteria are able to use sunlight to anabolically synthesize compounds from non living matter by photosynthesis nbsp Gluconeogenesis MechanismAnabolic pathway anabolism edit In contrast to catabolic pathways anabolic pathways require an energy input to construct macromolecules such as polypeptides nucleic acids proteins polysaccharides and lipids The isolated reaction of anabolism is unfavorable in a cell due to a positive Gibbs Free Energy DG Thus an input of chemical energy through a coupling with an exergonic reaction is necessary 1 25 27 The coupled reaction of the catabolic pathway affects the thermodynamics of the reaction by lowering the overall activation energy of an anabolic pathway and allowing the reaction to take place 1 25 Otherwise an endergonic reaction is non spontaneous An anabolic pathway is a biosynthetic pathway meaning that it combines smaller molecules to form larger and more complex ones 9 570 An example is the reversed pathway of glycolysis otherwise known as gluconeogenesis which occurs in the liver and sometimes in the kidney to maintain proper glucose concentration in the blood and supply the brain and muscle tissues with adequate amount of glucose Although gluconeogenesis is similar to the reverse pathway of glycolysis it contains four distinct enzymes pyruvate carboxylase phosphoenolpyruvate carboxykinase fructose 1 6 bisphosphatase glucose 6 phosphatase from glycolysis that allow the pathway to occur spontaneously 11 Amphibolic pathway edit nbsp Amphibolic Properties of the Citric Acid CycleAn amphibolic pathway is one that can be either catabolic or anabolic based on the availability of or the need for energy 9 570 The currency of energy in a biological cell is adenosine triphosphate ATP which stores its energy in the phosphoanhydride bonds The energy is utilized to conduct biosynthesis facilitate movement and regulate active transport inside of the cell 9 571 Examples of amphibolic pathways are the citric acid cycle and the glyoxylate cycle These sets of chemical reactions contain both energy producing and utilizing pathways 5 572 To the right is an illustration of the amphibolic properties of the TCA cycle The glyoxylate shunt pathway is an alternative to the tricarboxylic acid TCA cycle for it redirects the pathway of TCA to prevent full oxidation of carbon compounds and to preserve high energy carbon sources as future energy sources This pathway occurs only in plants and bacteria and transpires in the absence of glucose molecules 12 Regulation editThe flux of the entire pathway is regulated by the rate determining steps 1 577 578 These are the slowest steps in a network of reactions The rate limiting step occurs near the beginning of the pathway and is regulated by feedback inhibition which ultimately controls the overall rate of the pathway 13 The metabolic pathway in the cell is regulated by covalent or non covalent modifications A covalent modification involves an addition or removal of a chemical bond whereas a non covalent modification also known as allosteric regulation is the binding of the regulator to the enzyme via hydrogen bonds electrostatic interactions and Van Der Waals forces 14 The rate of turnover in a metabolic pathway also known as the metabolic flux is regulated based on the stoichiometric reaction model the utilization rate of metabolites and the translocation pace of molecules across the lipid bilayer 15 The regulation methods are based on experiments involving 13C labeling which is then analyzed by Nuclear Magnetic Resonance NMR or gas chromatography mass spectrometry GC MS derived mass compositions The aforementioned techniques synthesize a statistical interpretation of mass distribution in proteinogenic amino acids to the catalytic activities of enzymes in a cell 15 178 Clinical applications in targeting metabolic pathways editTargeting Oxidative Phosphorylation edit Metabolic pathways can be targeted for clinically therapeutic uses Within the mitochondrial metabolic network for instance there are various pathways that can be targeted by compounds to prevent cancer cell proliferation 16 One such pathway is oxidative phosphorylation OXPHOS within the electron transport chain ETC Various inhibitors can downregulate the electrochemical reactions that take place at Complex I II III and IV thereby preventing the formation of an electrochemical gradient and downregulating the movement of electrons through the ETC The substrate level phosphorylation that occurs at ATP synthase can also be directly inhibited preventing the formation of ATP that is necessary to supply energy for cancer cell proliferation 17 Some of these inhibitors such as lonidamine and atovaquone 16 which inhibit Complex II and Complex III respectively are currently undergoing clinical trials for FDA approval Other non FDA approved inhibitors have still shown experimental success in vitro Targeting Heme edit Heme an important prosthetic group present in Complexes I II and IV can also be targeted since heme biosynthesis and uptake have been correlated with increased cancer progression 18 Various molecules can inhibit heme via different mechanisms For instance succinylacetone has been shown to decrease heme concentrations by inhibiting d aminolevulinic acid in murine erythroleukemia cells 19 The primary structure of heme sequestering peptides such as HSP1 and HSP2 can be modified to downregulate heme concentrations and reduce proliferation of non small lung cancer cells 20 Targeting the Tricarboxylic acid cycle and Glutaminolysis edit The tricarboxylic acid cycle TCA and glutaminolysis can also be targeted for cancer treatment since they are essential for the survival and proliferation of cancer cells Ivosidenib and Enasidenib two FDA approved cancer treatments can arrest the TCA cycle of cancer cells by inhibiting isocitrate dehydrogenase 1 IDH1 and isocitrate dehydrogenase 2 IDH2 respectively 16 Ivosidenib is specific to acute myeloid leukemia AML and cholangiocarcinoma whereas Enasidenib is specific to just acute myeloid leukemia AML In a clinical trial consisting of 185 adult patients with cholangiocarcinoma and an IDH 1 mutation there was a statistically significant improvement p lt 0 0001 HR 0 37 in patients randomized to Ivosidenib Still some of the adverse side effects in these patients included fatigue nausea diarrhea decreased appetite ascites and anemia 21 In a clinical trial consisting of 199 adult patients with AML and an IDH2 mutation 23 of patients experienced complete response CR or complete response with partial hematologic recovery CRh lasting a median of 8 2 months while on Enasidenib Of the 157 patients who required transfusion at the beginning of the trial 34 no longer required transfusions during the 56 day time period on Enasidenib Of the 42 of patients who did not require transfusions at the beginning of the trial 76 still did not require a transfusion by the end of the trial Side effects of Enasidenib included nausea diarrhea elevated bilirubin and most notably differentiation syndrome 22 Glutaminase GLS the enzyme responsible for converting glutamine to glutamate via hydrolytic deamidation during the first reaction of glutaminolysis can also be targeted In recent years many small molecules such as azaserine acivicin and CB 839 have been shown to inhibit glutaminase thus reducing cancer cell viability and inducing apoptosis in cancer cells 23 Due to its effective antitumor ability in several cancer types such as ovarian breast and lung cancers CB 839 is the only GLS inhibitor currently undergoing clinical studies for FDA approval Genetic engineering of metabolic pathways editMany metabolic pathways are of commercial interest For instance the production of many antibiotics or other drugs requires complex pathways The pathways to produce such compounds can be transplanted into microbes or other more suitable organism for production purposes For example the world s supply of the anti cancer drug vinblastine is produced by relatively ineffient extraction and purification of the precursors vindoline and catharanthine from the plant Catharanthus roseus which are then chemically converted into vinblastine The biosynthetic pathway to produce vinblastine including 30 enzymatic steps has been transferred into yeast cells which is a convenient system to grow in large amounts With these genetic modifications yeast can use its own metabolites geranyl pyrophosphate and tryptophan to produce the precursors of catharanthine and vindoline This process required 56 genetic edits including expression of 34 heterologous genes from plants in yeast cells 24 See also editKaPPA View4 2010 Metabolism Metabolic control analysis Metabolic network Metabolic network modelling Metabolic engineering Biochemical systems equationReferences edit a b c d Nelson DL Cox MM 2008 Lehninger principles of biochemistry 5th ed New York W H Freeman ISBN 978 0 7167 7108 1 Alison S Papachristodoulou DK Despo K Elliott WH Elliott DC 2014 Biochemistry and molecular biology Fifth ed Oxford ISBN 978 0 19 960949 9 OCLC 862091499 a href Template Cite book html title Template Cite book cite book a CS1 maint location missing publisher link Nicholson DE March 1971 An Introduction to Metabolic Pathways by S DAGLEY Vol 59 No 2 ed Sigma Xi The Scientific Research Society p 266 a b Harvey RA 2011 Biochemistry 5th ed Baltimore MD Wolters Kluwer ISBN 978 1 60831 412 6 a b Voet D Voet JD Pratt CW 2013 Fundamentals of Biochemistry Life at the Molecular Level 4th ed Hoboken NJ Wiley ISBN 978 0470 54784 7 a b Reece JB Campbell NA 2011 Campbell Biology 9th ed Boston Benjamin Cummings Pearson pp 143 ISBN 978 0 321 55823 7 Berg JM Tymoczko JL Stryer L Gatto GJ 2012 Biochemistry 7th ed New York W H Freeman p 429 ISBN 978 1 4292 2936 4 Cornish Bowden A Cardenas M 2000 Irreversible reactions in metabolic simulations how reversible is irreversible PDF Animating the Cellular Map 65 71 a b c d Berg JM Tymoczko JL Stryer L 2002 Biochemistry 5th ed New York NY W H Freeman ISBN 978 0 7167 3051 4 Raven PH Evert RF Eichhorn SE 2011 Biology of plants 8th ed New York NY Freeman pp 100 106 ISBN 978 1 4292 1961 7 Berg JM Tymoczko JL Stryer L Gatto GJ 2012 Biochemistry 7th ed New York W H Freeman pp 480 482 ISBN 978 1 4292 2936 4 Pray L Relman DA Choffnes ER eds 2011 The science and applications of synthetic and systems biology workshop summary Washington D C National Academies Press p 135 ISBN 978 0 309 21939 6 Hill SA Ratcliffe RG 1999 Kruger NJ ed Regulation of primary metabolic pathways in plants proceedings of an international conference held on 9 11 January 1997 at St Hugh s College Oxford under the auspices of the Phytochemical Society of Europe Dordrecht u a Kluwer p 258 ISBN 978 0 7923 5494 9 White D 1995 The physiology and biochemistry of prokaryotes New York u a Oxford Univ Press p 133 ISBN 978 0 19 508439 9 a b Weckwerth W ed 2006 Metabolomics methods and protocols Totowa N J Humana Press p 177 ISBN 978 1 59745 244 1 a b c Frattaruolo L Brindisi M Curcio R Marra F Dolce V Cappello AR August 2020 Targeting the Mitochondrial Metabolic Network A Promising Strategy in Cancer Treatment International Journal of Molecular Sciences 21 17 2 11 doi 10 3390 ijms21176014 PMC 7503725 PMID 32825551 Yadav N Kumar S Marlowe T Chaudhary AK Kumar R Wang J et al November 2015 Oxidative phosphorylation dependent regulation of cancer cell apoptosis in response to anticancer agents Cell Death amp Disease 6 11 e1969 doi 10 1038 cddis 2015 305 PMC 4670921 PMID 26539916 Hooda J Cadinu D Alam MM Shah A Cao TM Sullivan LA et al 2013 Enhanced heme function and mitochondrial respiration promote the progression of lung cancer cells PLOS ONE 8 5 e63402 Bibcode 2013PLoSO 863402H doi 10 1371 journal pone 0063402 PMC 3660535 PMID 23704904 Ebert PS Hess RA Frykholm BC Tschudy DP June 1979 Succinylacetone a potent inhibitor of heme biosynthesis effect on cell growth heme content and delta aminolevulinic acid dehydratase activity of malignant murine erythroleukemia cells Biochemical and Biophysical Research Communications 88 4 1382 1390 doi 10 1016 0006 291x 79 91133 1 PMID 289386 Sohoni S Ghosh P Wang T Kalainayakan SP Vidal C Dey S et al May 2019 Elevated Heme Synthesis and Uptake Underpin Intensified Oxidative Metabolism and Tumorigenic Functions in Non Small Cell Lung Cancer Cells Cancer Research 79 10 2511 2525 doi 10 1158 0008 5472 CAN 18 2156 PMID 30902795 S2CID 85456667 FDA approves Ivosidenib for advanced or metastatic cholangiocarcinoma U S Food amp Drug Administration 26 August 2021 FDA granted regular approval to enasidenib for the treatment of relapsed or refractory AML U S Food amp Drug Administration 9 February 2019 Mates JM Di Paola FJ Campos Sandoval JA Mazurek S Marquez J February 2020 Therapeutic targeting of glutaminolysis as an essential strategy to combat cancer Seminars in Cell amp Developmental Biology 98 34 43 doi 10 1016 j semcdb 2019 05 012 PMID 31100352 S2CID 157067127 Zhang J Hansen LG Gudich O Viehrig K Lassen LM Schrubbers L et al September 2022 A microbial supply chain for production of the anti cancer drug vinblastine Nature 609 7926 341 347 Bibcode 2022Natur 609 341Z doi 10 1038 s41586 022 05157 3 PMC 9452304 PMID 36045295 External links edit nbsp Wikimedia Commons has media related to Metabolic pathways Full map of metabolic pathways Biochemical pathways Gerhard Michal Overview Map from BRENDA BioCyc Metabolic network models for thousands of sequenced organisms KEGG Kyoto Encyclopedia of Genes and Genomes Reactome a database of reactions pathways and biological processes MetaCyc A database of experimentally elucidated metabolic pathways 2 200 pathways from more than 2 500 organisms MetaboMAPS A platform for pathway sharing and data visualization on metabolic pathways The Pathway Localization database PathLocdb DAVID Visualize genes on pathway maps Wikipathways pathways for the people ConsensusPathDB metpath Integrated interactive metabolic chartMetabolic pathway diagram nbsp Glucuronate metabolism Pentose interconversion Inositol metabolism Cellulose and sucrosemetabolism Starch and glycogenmetabolism Other sugarmetabolism Pentose phosphate pathway Glycolysis and Gluconeogenesis Amino sugars metabolism Small amino acid synthesis Branched amino acidsynthesis Purine biosynthesis Histidine metabolism Aromatic aminoacid synthesis Pyruvatedecarboxylation Fermentation Fatty acidmetabolism Urea cycle Aspartate amino acidgroup synthesis Porphyrins andcorrinoidsmetabolism Citric acid cycle Glutamate aminoacid groupsynthesis Pyrimidine biosynthesis vte nbsp All pathway labels on this image are links simply click to access the article A high resolution labeled version of this image is available here nbsp Retrieved from https en wikipedia org w index php title Metabolic pathway amp oldid 1179938981, wikipedia, wiki, book, books, library,

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