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Adenosine triphosphate

January 26, 2023

Adenosine triphosphate (ATP) is an organic compound that provides energy to drive many processes in living cells, such as muscle contraction, nerve impulse propagation, condensate dissolution, and chemical synthesis. Found in all known forms of life, ATP is often referred to as the "molecular unit of currency" of intracellular energy transfer.[2] When consumed in metabolic processes, it converts either to adenosine diphosphate (ADP) or to adenosine monophosphate (AMP). Other processes regenerate ATP. The human body recycles its own body weight equivalent in ATP each day.[3] It is also a precursor to DNA and RNA, and is used as a coenzyme.

Adenosine-5'-triphosphate
Names
IUPAC name
Adenosine 5′-(tetrahydrogen triphosphate)
Preferred IUPAC name
O1-{[(2R,3S,4R,5R)-5-(6-Amino-9H-purin-9-yl)-3,4-dihydroxyoxolan-2-yl]methyl} tetrahydrogen triphosphate
Identifiers
  • 56-65-5 (free acid) Y
  • 34369-07-8 (disodium salt hydrate) N
3D model (JSmol)
  • Interactive image
  • Interactive image
ChEBI
  • CHEBI:15422 Y
ChEMBL
  • ChEMBL14249 Y
ChemSpider
  • 5742 Y
DrugBank
  • DB00171 Y
ECHA InfoCard 100.000.258
  • 1713
KEGG
  • C00002 Y
  • 5957
UNII
  • 8L70Q75FXE Y
  • DTXSID6022559
  • InChI=1S/C10H16N5O13P3/c11-8-5-9(13-2-12-8)15(3-14-5)10-7(17)6(16)4(26-10)1-25-30(21,22)28-31(23,24)27-29(18,19)20/h2-4,6-7,10,16-17H,1H2,(H,21,22)(H,23,24)(H2,11,12,13)(H2,18,19,20)/t4-,6-,7-,10-/m1/s1 Y
    Key: ZKHQWZAMYRWXGA-KQYNXXCUSA-N Y
  • Key: ZKHQWZAMYRWXGA-KQYNXXCUBG
  • O=P(O)(O)OP(=O)(O)OP(=O)(O)OC[C@H]3O[C@@H](n2cnc1c(ncnc12)N)[C@H](O)[C@@H]3O
  • c1nc(c2c(n1)n(cn2)[C@H]3[C@@H]([C@@H]([C@H](O3)COP(=O)(O)OP(=O)(O)OP(=O)(O)O)O)O)N
Properties
C10H16N5O13P3
Molar mass 507.18 g/mol
Density 1.04 g/cm3 (disodium salt)
Melting point 187 °C (369 °F; 460 K) disodium salt; decomposes
Acidity (pKa) 0.9, 1.4, 3.8, 6.5
UV-vismax) 259 nm[1]
Absorbance ε259 = 15.4 mM−1 cm−1 [1]
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa).
Y verify (what is YN ?)
Interactive animation of the structure of ATP

From the perspective of biochemistry, ATP is classified as a nucleoside triphosphate, which indicates that it consists of three components: a nitrogenous base (adenine), the sugar ribose, and the triphosphate.

Structure

ATP consists of an adenine attached by the 9-nitrogen atom to the 1′ carbon atom of a sugar (ribose), which in turn is attached at the 5' carbon atom of the sugar to a triphosphate group. In its many reactions related to metabolism, the adenine and sugar groups remain unchanged, but the triphosphate is converted to di- and monophosphate, giving respectively the derivatives ADP and AMP. The three phosphoryl groups are labeled as alpha (α), beta (β), and, for the terminal phosphate, gamma (γ).

In neutral solution, ionized ATP exists mostly as ATP4−, with a small proportion of ATP3−.[4]

Binding of metal cations to ATP

Being polyanionic and featuring a potentially chelating polyphosphate group, ATP binds metal cations with high affinity. The binding constant for Mg2+
 is (9554).[5] The binding of a divalent cation, almost always magnesium, strongly affects the interaction of ATP with various proteins. Due to the strength of the ATP-Mg2+ interaction, ATP exists in the cell mostly as a complex with Mg2+
 bonded to the phosphate oxygen centers.[4][6]

A second magnesium ion is critical for ATP binding in the kinase domain.[7] The presence of Mg2+ regulates kinase activity.[8]

Chemical properties

Salts of ATP can be isolated as colorless solids.[9]

 
The cycles of synthesis and degradation of ATP; 2 and 1 represent input and output of energy, respectively.

ATP is stable in aqueous solutions between pH 6.8 and 7.4, in the absence of catalysts. At more extreme pHs, it rapidly hydrolyses to ADP and phosphate. Living cells maintain the ratio of ATP to ADP at a point ten orders of magnitude from equilibrium, with ATP concentrations fivefold higher than the concentration of ADP.[10][11] In the context of biochemical reactions, the P-O-P bonds are frequently referred to as high-energy bonds.[12]

Reactive aspects

The hydrolysis of ATP into ADP and inorganic phosphate releases 20.5 kJ/mol of enthalpy.[13] The values of the free energy released by cleaving either a phosphate (Pi) or a pyrophosphate (PPi) unit from ATP at standard state concentrations of 1 mol/L at pH 7 are:[14]

ATP + H
2O → ADP + Pi   ΔG°' = −30.5 kJ/mol (−7.3 kcal/mol)
ATP + H
2O → AMP + PPi  ΔG°' = −45.6 kJ/mol (−10.9 kcal/mol)

These abbreviated equations at a pH near 7 can be written more explicitly (R = adenosyl):

[RO-P(O)2-O-P(O)2-O-PO3]4− + H
2O → [RO-P(O)2-O-PO3]3− + [HPO4]2− + H+
[RO-P(O)2-O-P(O)2-O-PO3]4− + H
2O → [RO-PO3]2− + [HO3P-O-PO3]3− + H+

At cytoplasmic conditions, where the ADP/ATP ratio is 10 orders of magnitude from equilibrium, the ΔG is around −57 kJ/mol.[10]

 
This image shows a 360-degree rotation of a single, gas-phase magnesium-ATP chelate with a charge of −2. The anion was optimized at the UB3LYP/6-311++G(d,p) theoretical level and the atomic connectivity modified by the human optimizer to reflect the probable electronic structure.

Production from AMP and ADP

Production, aerobic conditions

A typical intracellular concentration of ATP is hard to pin down, however, reports have shown there to be 1–10 μmol per gram of tissue in a variety of eukaryotes.[15] The dephosphorylation of ATP and rephosphorylation of ADP and AMP occur repeatedly in the course of aerobic metabolism.

ATP can be produced by a number of distinct cellular processes; the three main pathways in eukaryotes are (1) glycolysis, (2) the citric acid cycle/oxidative phosphorylation, and (3) beta-oxidation. The overall process of oxidizing glucose to carbon dioxide, the combination of pathways 1 and 2, known as cellular respiration, produces about 30 equivalents of ATP from each molecule of glucose.[16]

ATP production by a non-photosynthetic aerobic eukaryote occurs mainly in the mitochondria, which comprise nearly 25% of the volume of a typical cell.[17]

Glycolysis

Main article: Glycolysis

In glycolysis, glucose and glycerol are metabolized to pyruvate. Glycolysis generates two equivalents of ATP through substrate phosphorylation catalyzed by two enzymes, phosphoglycerate kinase (PGK) and pyruvate kinase. Two equivalents of nicotinamide adenine dinucleotide (NADH) are also produced, which can be oxidized via the electron transport chain and result in the generation of additional ATP by ATP synthase. The pyruvate generated as an end-product of glycolysis is a substrate for the Krebs Cycle.[18]

Glycolysis is viewed as consisting of two phases with five steps each. In phase 1, "the preparatory phase", glucose is converted to 2 d-glyceraldehyde-3-phosphate (g3p). One ATP is invested in Step 1, and another ATP is invested in Step 3. Steps 1 and 3 of glycolysis are referred to as "Priming Steps". In Phase 2, two equivalents of g3p are converted to two pyruvates. In Step 7, two ATP are produced. Also, in Step 10, two further equivalents of ATP are produced. In Steps 7 and 10, ATP is generated from ADP. A net of two ATPs is formed in the glycolysis cycle. The glycolysis pathway is later associated with the Citric Acid Cycle which produces additional equivalents of ATP.

Regulation

In glycolysis, hexokinase is directly inhibited by its product, glucose-6-phosphate, and pyruvate kinase is inhibited by ATP itself. The main control point for the glycolytic pathway is phosphofructokinase (PFK), which is allosterically inhibited by high concentrations of ATP and activated by high concentrations of AMP. The inhibition of PFK by ATP is unusual since ATP is also a substrate in the reaction catalyzed by PFK; the active form of the enzyme is a tetramer that exists in two conformations, only one of which binds the second substrate fructose-6-phosphate (F6P). The protein has two binding sites for ATP – the active site is accessible in either protein conformation, but ATP binding to the inhibitor site stabilizes the conformation that binds F6P poorly.[18] A number of other small molecules can compensate for the ATP-induced shift in equilibrium conformation and reactivate PFK, including cyclic AMP, ammonium ions, inorganic phosphate, and fructose-1,6- and -2,6-biphosphate.[18]

Citric acid cycle

Main articles: Citric acid cycle and Oxidative phosphorylation

In the mitochondrion, pyruvate is oxidized by the pyruvate dehydrogenase complex to the acetyl group, which is fully oxidized to carbon dioxide by the citric acid cycle (also known as the Krebs cycle). Every "turn" of the citric acid cycle produces two molecules of carbon dioxide, one equivalent of ATP guanosine triphosphate (GTP) through substrate-level phosphorylation catalyzed by succinyl-CoA synthetase, as succinyl-CoA is converted to succinate, three equivalents of NADH, and one equivalent of FADH2. NADH and FADH2 are recycled (to NAD+ and FAD, respectively) by oxidative phosphorylation, generating additional ATP. The oxidation of NADH results in the synthesis of 2–3 equivalents of ATP, and the oxidation of one FADH2 yields between 1–2 equivalents of ATP.[16] The majority of cellular ATP is generated by this process. Although the citric acid cycle itself does not involve molecular oxygen, it is an obligately aerobic process because O2 is used to recycle the NADH and FADH2. In the absence of oxygen, the citric acid cycle ceases.[17]

The generation of ATP by the mitochondrion from cytosolic NADH relies on the malate-aspartate shuttle (and to a lesser extent, the glycerol-phosphate shuttle) because the inner mitochondrial membrane is impermeable to NADH and NAD+. Instead of transferring the generated NADH, a malate dehydrogenase enzyme converts oxaloacetate to malate, which is translocated to the mitochondrial matrix. Another malate dehydrogenase-catalyzed reaction occurs in the opposite direction, producing oxaloacetate and NADH from the newly transported malate and the mitochondrion's interior store of NAD+. A transaminase converts the oxaloacetate to aspartate for transport back across the membrane and into the intermembrane space.[17]

In oxidative phosphorylation, the passage of electrons from NADH and FADH2 through the electron transport chain releases the energy to pump protons out of the mitochondrial matrix and into the intermembrane space. This pumping generates a proton motive force that is the net effect of a pH gradient and an electric potential gradient across the inner mitochondrial membrane. Flow of protons down this potential gradient – that is, from the intermembrane space to the matrix – yields ATP by ATP synthase.[19] Three ATP are produced per turn.

Although oxygen consumption appears fundamental for the maintenance of the proton motive force, in the event of oxygen shortage (hypoxia), intracellular acidosis (mediated by enhanced glycolytic rates and ATP hydrolysis), contributes to mitochondrial membrane potential and directly drives ATP synthesis.[20]

Most of the ATP synthesized in the mitochondria will be used for cellular processes in the cytosol; thus it must be exported from its site of synthesis in the mitochondrial matrix. ATP outward movement is favored by the membrane's electrochemical potential because the cytosol has a relatively positive charge compared to the relatively negative matrix. For every ATP transported out, it costs 1 H+. Producing one ATP costs about 3 H+. Therefore, making and exporting one ATP requires 4H+. The inner membrane contains an antiporter, the ADP/ATP translocase, which is an integral membrane protein used to exchange newly synthesized ATP in the matrix for ADP in the intermembrane space.[21] This translocase is driven by the membrane potential, as it results in the movement of about 4 negative charges out across the mitochondrial membrane in exchange for 3 negative charges moved inside. However, it is also necessary to transport phosphate into the mitochondrion; the phosphate carrier moves a proton in with each phosphate, partially dissipating the proton gradient. After completing glycolysis, the citric acid cycle, the electron transport chain, and oxidative phosphorylation, approximately 30–38 ATP molecules are produced per glucose.

Regulation

The citric acid cycle is regulated mainly by the availability of key substrates, particularly the ratio of NAD+ to NADH and the concentrations of calcium, inorganic phosphate, ATP, ADP, and AMP. Citrate – the ion that gives its name to the cycle – is a feedback inhibitor of citrate synthase and also inhibits PFK, providing a direct link between the regulation of the citric acid cycle and glycolysis.[18]

Beta oxidation

Main article: Beta-oxidation

In the presence of air and various cofactors and enzymes, fatty acids are converted to acetyl-CoA. The pathway is called beta-oxidation. Each cycle of beta-oxidation shortens the fatty acid chain by two carbon atoms and produces one equivalent each of acetyl-CoA, NADH, and FADH2. The acetyl-CoA is metabolized by the citric acid cycle to generate ATP, while the NADH and FADH2 are used by oxidative phosphorylation to generate ATP. Dozens of ATP equivalents are generated by the beta-oxidation of a single long acyl chain.[22]

Regulation

In oxidative phosphorylation, the key control point is the reaction catalyzed by cytochrome c oxidase, which is regulated by the availability of its substrate – the reduced form of cytochrome c. The amount of reduced cytochrome c available is directly related to the amounts of other substrates:

 

which directly implies this equation:

 

Thus, a high ratio of [NADH] to [NAD+] or a high ratio of [ADP][Pi] to [ATP] imply a high amount of reduced cytochrome c and a high level of cytochrome c oxidase activity.[18] An additional level of regulation is introduced by the transport rates of ATP and NADH between the mitochondrial matrix and the cytoplasm.[21]

Ketosis

Main article: Ketone bodies

Ketone bodies can be used as fuels, yielding 22 ATP and 2 GTP molecules per acetoacetate molecule when oxidized in the mitochondria. Ketone bodies are transported from the liver to other tissues, where acetoacetate and beta-hydroxybutyrate can be reconverted to acetyl-CoA to produce reducing equivalents (NADH and FADH2), via the citric acid cycle. Ketone bodies cannot be used as fuel by the liver, because the liver lacks the enzyme β-ketoacyl-CoA transferase, also called thiolase. Acetoacetate in low concentrations is taken up by the liver and undergoes detoxification through the methylglyoxal pathway which ends with lactate. Acetoacetate in high concentrations is absorbed by cells other than those in the liver and enters a different pathway via 1,2-propanediol. Though the pathway follows a different series of steps requiring ATP, 1,2-propanediol can be turned into pyruvate.[23]

Production, anaerobic conditions

Fermentation is the metabolism of organic compounds in the absence of air. It involves substrate-level phosphorylation in the absence of a respiratory electron transport chain. The equation for the reaction of glucose to form lactic acid is:

C
6H
12O
6 + 2 ADP + 2 Pi → 2 CH
3CH(OH)COOH + 2 ATP + 2 H
2O

Anaerobic respiration is respiration in the absence of O
2. Prokaryotes can utilize a variety of electron acceptors. These include nitrate, sulfate, and carbon dioxide.

ATP replenishment by nucleoside diphosphate kinases

ATP can also be synthesized through several so-called "replenishment" reactions catalyzed by the enzyme families of nucleoside diphosphate kinases (NDKs), which use other nucleoside triphosphates as a high-energy phosphate donor, and the ATP:guanido-phosphotransferase family.

ATP production during photosynthesis

In plants, ATP is synthesized in the thylakoid membrane of the chloroplast. The process is called photophosphorylation. The "machinery" is similar to that in mitochondria except that light energy is used to pump protons across a membrane to produce a proton-motive force. ATP synthase then ensues exactly as in oxidative phosphorylation.[24] Some of the ATP produced in the chloroplasts is consumed in the Calvin cycle, which produces triose sugars.

ATP recycling

The total quantity of ATP in the human body is about 0.1 mol/L.[25] The majority of ATP is recycled from ADP by the aforementioned processes. Thus, at any given time, the total amount of ATP + ADP remains fairly constant.

The energy used by human cells in an adult requires the hydrolysis of 100 to 150 mol/L of ATP daily, which means a human will typically use their body weight worth of ATP over the course of the day.[26] Each equivalent of ATP is recycled 1000–1500 times during a single day (150 / 0.1 = 1500),[25] at approximately 9×1020 molecules/s.[25]

 
An example of the Rossmann fold, a structural domain of a decarboxylase enzyme from the bacterium Staphylococcus epidermidis (PDB: 1G5Q​) with a bound flavin mononucleotide cofactor.

Biochemical functions

Intracellular signaling

ATP is involved in signal transduction by serving as substrate for kinases, enzymes that transfer phosphate groups. Kinases are the most common ATP-binding proteins. They share a small number of common folds.[27] Phosphorylation of a protein by a kinase can activate a cascade such as the mitogen-activated protein kinase cascade.[28]

ATP is also a substrate of adenylate cyclase, most commonly in G protein-coupled receptor signal transduction pathways and is transformed to second messenger, cyclic AMP, which is involved in triggering calcium signals by the release of calcium from intracellular stores.[29] This form of signal transduction is particularly important in brain function, although it is involved in the regulation of a multitude of other cellular processes.[30]

DNA and RNA synthesis

ATP is one of four monomers required in the synthesis of RNA. The process is promoted by RNA polymerases.[31] A similar process occurs in the formation of DNA, except that ATP is first converted to the deoxyribonucleotide dATP. Like many condensation reactions in nature, DNA replication and DNA transcription also consume ATP.

Amino acid activation in protein synthesis

Main article: Amino acid activation

Aminoacyl-tRNA synthetase enzymes consume ATP in the attachment tRNA to amino acids, forming aminoacyl-tRNA complexes. Aminoacyl transferase binds AMP-amino acid to tRNA. The coupling reaction proceeds in two steps:

  1. aa + ATP ⟶ aa-AMP + PPi
  2. aa-AMP + tRNA ⟶ aa-tRNA + AMP

The amino acid is coupled to the penultimate nucleotide at the 3′-end of the tRNA (the A in the sequence CCA) via an ester bond (roll over in illustration).

ATP binding cassette transporter

Transporting chemicals out of a cell against a gradient is often associated with ATP hydrolysis. Transport is mediated by ATP binding cassette transporters. The human genome encodes 48 ABC transporters, that are used for exporting drugs, lipids, and other compounds.[32]

Extracellular signalling and neurotransmission

Cells secrete ATP to communicate with other cells in a process called purinergic signalling. ATP serves as a neurotransmitter in many parts of the nervous system, modulates ciliary beating, affects vascular oxygen supply etc. ATP is either secreted directly across the cell membrane through channel proteins[33][34] or is pumped into vesicles[35] which then fuse with the membrane. Cells detect ATP using the purinergic receptor proteins P2X and P2Y.

Protein solubility

ATP has recently been proposed to act as a biological hydrotrope[36] and has been shown to affect proteome-wide solubility.[37]

ATP analogues

Biochemistry laboratories often use in vitro studies to explore ATP-dependent molecular processes. ATP analogs are also used in X-ray crystallography to determine a protein structure in complex with ATP, often together with other substrates.

Enzyme inhibitors of ATP-dependent enzymes such as kinases are needed to examine the binding sites and transition states involved in ATP-dependent reactions.

Most useful ATP analogs cannot be hydrolyzed as ATP would be; instead, they trap the enzyme in a structure closely related to the ATP-bound state. Adenosine 5′-(γ-thiotriphosphate) is an extremely common ATP analog in which one of the gamma-phosphate oxygens is replaced by a sulfur atom; this anion is hydrolyzed at a dramatically slower rate than ATP itself and functions as an inhibitor of ATP-dependent processes. In crystallographic studies, hydrolysis transition states are modeled by the bound vanadate ion.

Caution is warranted in interpreting the results of experiments using ATP analogs, since some enzymes can hydrolyze them at appreciable rates at high concentration.[38]

Medical use

ATP is used intravenously for some heart related conditions.[39]

History

ATP was discovered in 1929 by Karl Lohmann[40] and Jendrassik[41] and, independently, by Cyrus Fiske and Yellapragada Subba Rao of Harvard Medical School,[42] both teams competing against each other to find an assay for phosphorus.

It was proposed to be the intermediary between energy-yielding and energy-requiring reactions in cells by Fritz Albert Lipmann in 1941.[43]

It was first synthesized in the laboratory by Alexander Todd in 1948,[44] and he was awarded the Nobel Prize in Chemistry in 1957 partly for this work.

The 1978 Nobel Prize in Chemistry was awarded to Dr. Peter Dennis Mitchell for the discovery of the chemiosmotic mechanism of ATP synthesis.

The 1997 Nobel Prize in Chemistry was divided, one half jointly to Paul D. Boyer and John E. Walker "for their elucidation of the enzymatic mechanism underlying the synthesis of adenosine triphosphate (ATP)" and the other half to Jens C. Skou "for the first discovery of an ion-transporting enzyme, Na+, K+ -ATPase."[45]

See also

References

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External links

 
Wikimedia Commons has media related to Adenosine triphosphate.
  • ATP bound to proteins in the PDB
  • PubChem entry for Adenosine Triphosphate
  • KEGG entry for Adenosine Triphosphate

January 26, 2023
adenosine, triphosphate, organic, compound, that, provides, energy, drive, many, processes, living, cells, such, muscle, contraction, nerve, impulse, propagation, condensate, dissolution, chemical, synthesis, found, known, forms, life, often, referred, molecul. Adenosine triphosphate ATP is an organic compound that provides energy to drive many processes in living cells such as muscle contraction nerve impulse propagation condensate dissolution and chemical synthesis Found in all known forms of life ATP is often referred to as the molecular unit of currency of intracellular energy transfer 2 When consumed in metabolic processes it converts either to adenosine diphosphate ADP or to adenosine monophosphate AMP Other processes regenerate ATP The human body recycles its own body weight equivalent in ATP each day 3 It is also a precursor to DNA and RNA and is used as a coenzyme Adenosine 5 triphosphate NamesIUPAC name Adenosine 5 tetrahydrogen triphosphate Preferred IUPAC name O1 2R 3S 4R 5R 5 6 Amino 9H purin 9 yl 3 4 dihydroxyoxolan 2 yl methyl tetrahydrogen triphosphateIdentifiersCAS Number 56 65 5 free acid Y34369 07 8 disodium salt hydrate N3D model JSmol Interactive imageInteractive imageChEBI CHEBI 15422 YChEMBL ChEMBL14249 YChemSpider 5742 YDrugBank DB00171 YECHA InfoCard 100 000 258IUPHAR BPS 1713KEGG C00002 YPubChem CID 5957UNII 8L70Q75FXE YCompTox Dashboard EPA DTXSID6022559InChI InChI 1S C10H16N5O13P3 c11 8 5 9 13 2 12 8 15 3 14 5 10 7 17 6 16 4 26 10 1 25 30 21 22 28 31 23 24 27 29 18 19 20 h2 4 6 7 10 16 17H 1H2 H 21 22 H 23 24 H2 11 12 13 H2 18 19 20 t4 6 7 10 m1 s1 YKey ZKHQWZAMYRWXGA KQYNXXCUSA N YKey ZKHQWZAMYRWXGA KQYNXXCUBGSMILES O P O O OP O O OP O O OC C H 3O C H n2cnc1c ncnc12 N C H O C H 3Oc1nc c2c n1 n cn2 C H 3 C H C H C H O3 COP O O OP O O OP O O O O O NPropertiesChemical formula C 10H 16N 5O 13P 3Molar mass 507 18 g molDensity 1 04 g cm3 disodium salt Melting point 187 C 369 F 460 K disodium salt decomposesAcidity pKa 0 9 1 4 3 8 6 5UV vis lmax 259 nm 1 Absorbance e259 15 4 mM 1 cm 1 1 Except where otherwise noted data are given for materials in their standard state at 25 C 77 F 100 kPa Y verify what is Y N Infobox references Interactive animation of the structure of ATP From the perspective of biochemistry ATP is classified as a nucleoside triphosphate which indicates that it consists of three components a nitrogenous base adenine the sugar ribose and the triphosphate Contents 1 Structure 1 1 Binding of metal cations to ATP 2 Chemical properties 3 Reactive aspects 4 Production from AMP and ADP 4 1 Production aerobic conditions 4 1 1 Glycolysis 4 1 1 1 Regulation 4 1 2 Citric acid cycle 4 1 2 1 Regulation 4 1 3 Beta oxidation 4 1 3 1 Regulation 4 1 4 Ketosis 4 2 Production anaerobic conditions 4 2 1 ATP replenishment by nucleoside diphosphate kinases 4 3 ATP production during photosynthesis 4 4 ATP recycling 5 Biochemical functions 5 1 Intracellular signaling 5 2 DNA and RNA synthesis 5 3 Amino acid activation in protein synthesis 5 4 ATP binding cassette transporter 5 5 Extracellular signalling and neurotransmission 5 6 Protein solubility 6 ATP analogues 7 Medical use 8 History 9 See also 10 References 11 External linksStructure EditATP consists of an adenine attached by the 9 nitrogen atom to the 1 carbon atom of a sugar ribose which in turn is attached at the 5 carbon atom of the sugar to a triphosphate group In its many reactions related to metabolism the adenine and sugar groups remain unchanged but the triphosphate is converted to di and monophosphate giving respectively the derivatives ADP and AMP The three phosphoryl groups are labeled as alpha a beta b and for the terminal phosphate gamma g In neutral solution ionized ATP exists mostly as ATP4 with a small proportion of ATP3 4 Binding of metal cations to ATP Edit Being polyanionic and featuring a potentially chelating polyphosphate group ATP binds metal cations with high affinity The binding constant for Mg2 is 9554 5 The binding of a divalent cation almost always magnesium strongly affects the interaction of ATP with various proteins Due to the strength of the ATP Mg2 interaction ATP exists in the cell mostly as a complex with Mg2 bonded to the phosphate oxygen centers 4 6 A second magnesium ion is critical for ATP binding in the kinase domain 7 The presence of Mg2 regulates kinase activity 8 Chemical properties EditSalts of ATP can be isolated as colorless solids 9 The cycles of synthesis and degradation of ATP 2 and 1 represent input and output of energy respectively ATP is stable in aqueous solutions between pH 6 8 and 7 4 in the absence of catalysts At more extreme pHs it rapidly hydrolyses to ADP and phosphate Living cells maintain the ratio of ATP to ADP at a point ten orders of magnitude from equilibrium with ATP concentrations fivefold higher than the concentration of ADP 10 11 In the context of biochemical reactions the P O P bonds are frequently referred to as high energy bonds 12 Reactive aspects EditThe hydrolysis of ATP into ADP and inorganic phosphate releases 20 5 kJ mol of enthalpy 13 The values of the free energy released by cleaving either a phosphate Pi or a pyrophosphate PPi unit from ATP at standard state concentrations of 1 mol L at pH 7 are 14 ATP H2 O ADP Pi DG 30 5 kJ mol 7 3 kcal mol ATP H2 O AMP PPi DG 45 6 kJ mol 10 9 kcal mol These abbreviated equations at a pH near 7 can be written more explicitly R adenosyl RO P O 2 O P O 2 O PO3 4 H2 O RO P O 2 O PO3 3 HPO4 2 H RO P O 2 O P O 2 O PO3 4 H2 O RO PO3 2 HO3P O PO3 3 H At cytoplasmic conditions where the ADP ATP ratio is 10 orders of magnitude from equilibrium the DG is around 57 kJ mol 10 This image shows a 360 degree rotation of a single gas phase magnesium ATP chelate with a charge of 2 The anion was optimized at the UB3LYP 6 311 G d p theoretical level and the atomic connectivity modified by the human optimizer to reflect the probable electronic structure Production from AMP and ADP EditProduction aerobic conditions Edit A typical intracellular concentration of ATP is hard to pin down however reports have shown there to be 1 10 mmol per gram of tissue in a variety of eukaryotes 15 The dephosphorylation of ATP and rephosphorylation of ADP and AMP occur repeatedly in the course of aerobic metabolism ATP can be produced by a number of distinct cellular processes the three main pathways in eukaryotes are 1 glycolysis 2 the citric acid cycle oxidative phosphorylation and 3 beta oxidation The overall process of oxidizing glucose to carbon dioxide the combination of pathways 1 and 2 known as cellular respiration produces about 30 equivalents of ATP from each molecule of glucose 16 ATP production by a non photosynthetic aerobic eukaryote occurs mainly in the mitochondria which comprise nearly 25 of the volume of a typical cell 17 Glycolysis Edit Main article Glycolysis In glycolysis glucose and glycerol are metabolized to pyruvate Glycolysis generates two equivalents of ATP through substrate phosphorylation catalyzed by two enzymes phosphoglycerate kinase PGK and pyruvate kinase Two equivalents of nicotinamide adenine dinucleotide NADH are also produced which can be oxidized via the electron transport chain and result in the generation of additional ATP by ATP synthase The pyruvate generated as an end product of glycolysis is a substrate for the Krebs Cycle 18 Glycolysis is viewed as consisting of two phases with five steps each In phase 1 the preparatory phase glucose is converted to 2 d glyceraldehyde 3 phosphate g3p One ATP is invested in Step 1 and another ATP is invested in Step 3 Steps 1 and 3 of glycolysis are referred to as Priming Steps In Phase 2 two equivalents of g3p are converted to two pyruvates In Step 7 two ATP are produced Also in Step 10 two further equivalents of ATP are produced In Steps 7 and 10 ATP is generated from ADP A net of two ATPs is formed in the glycolysis cycle The glycolysis pathway is later associated with the Citric Acid Cycle which produces additional equivalents of ATP Regulation Edit In glycolysis hexokinase is directly inhibited by its product glucose 6 phosphate and pyruvate kinase is inhibited by ATP itself The main control point for the glycolytic pathway is phosphofructokinase PFK which is allosterically inhibited by high concentrations of ATP and activated by high concentrations of AMP The inhibition of PFK by ATP is unusual since ATP is also a substrate in the reaction catalyzed by PFK the active form of the enzyme is a tetramer that exists in two conformations only one of which binds the second substrate fructose 6 phosphate F6P The protein has two binding sites for ATP the active site is accessible in either protein conformation but ATP binding to the inhibitor site stabilizes the conformation that binds F6P poorly 18 A number of other small molecules can compensate for the ATP induced shift in equilibrium conformation and reactivate PFK including cyclic AMP ammonium ions inorganic phosphate and fructose 1 6 and 2 6 biphosphate 18 Citric acid cycle Edit Main articles Citric acid cycle and Oxidative phosphorylation In the mitochondrion pyruvate is oxidized by the pyruvate dehydrogenase complex to the acetyl group which is fully oxidized to carbon dioxide by the citric acid cycle also known as the Krebs cycle Every turn of the citric acid cycle produces two molecules of carbon dioxide one equivalent of ATP guanosine triphosphate GTP through substrate level phosphorylation catalyzed by succinyl CoA synthetase as succinyl CoA is converted to succinate three equivalents of NADH and one equivalent of FADH2 NADH and FADH2 are recycled to NAD and FAD respectively by oxidative phosphorylation generating additional ATP The oxidation of NADH results in the synthesis of 2 3 equivalents of ATP and the oxidation of one FADH2 yields between 1 2 equivalents of ATP 16 The majority of cellular ATP is generated by this process Although the citric acid cycle itself does not involve molecular oxygen it is an obligately aerobic process because O2 is used to recycle the NADH and FADH2 In the absence of oxygen the citric acid cycle ceases 17 The generation of ATP by the mitochondrion from cytosolic NADH relies on the malate aspartate shuttle and to a lesser extent the glycerol phosphate shuttle because the inner mitochondrial membrane is impermeable to NADH and NAD Instead of transferring the generated NADH a malate dehydrogenase enzyme converts oxaloacetate to malate which is translocated to the mitochondrial matrix Another malate dehydrogenase catalyzed reaction occurs in the opposite direction producing oxaloacetate and NADH from the newly transported malate and the mitochondrion s interior store of NAD A transaminase converts the oxaloacetate to aspartate for transport back across the membrane and into the intermembrane space 17 In oxidative phosphorylation the passage of electrons from NADH and FADH2 through the electron transport chain releases the energy to pump protons out of the mitochondrial matrix and into the intermembrane space This pumping generates a proton motive force that is the net effect of a pH gradient and an electric potential gradient across the inner mitochondrial membrane Flow of protons down this potential gradient that is from the intermembrane space to the matrix yields ATP by ATP synthase 19 Three ATP are produced per turn Although oxygen consumption appears fundamental for the maintenance of the proton motive force in the event of oxygen shortage hypoxia intracellular acidosis mediated by enhanced glycolytic rates and ATP hydrolysis contributes to mitochondrial membrane potential and directly drives ATP synthesis 20 Most of the ATP synthesized in the mitochondria will be used for cellular processes in the cytosol thus it must be exported from its site of synthesis in the mitochondrial matrix ATP outward movement is favored by the membrane s electrochemical potential because the cytosol has a relatively positive charge compared to the relatively negative matrix For every ATP transported out it costs 1 H Producing one ATP costs about 3 H Therefore making and exporting one ATP requires 4H The inner membrane contains an antiporter the ADP ATP translocase which is an integral membrane protein used to exchange newly synthesized ATP in the matrix for ADP in the intermembrane space 21 This translocase is driven by the membrane potential as it results in the movement of about 4 negative charges out across the mitochondrial membrane in exchange for 3 negative charges moved inside However it is also necessary to transport phosphate into the mitochondrion the phosphate carrier moves a proton in with each phosphate partially dissipating the proton gradient After completing glycolysis the citric acid cycle the electron transport chain and oxidative phosphorylation approximately 30 38 ATP molecules are produced per glucose Regulation Edit The citric acid cycle is regulated mainly by the availability of key substrates particularly the ratio of NAD to NADH and the concentrations of calcium inorganic phosphate ATP ADP and AMP Citrate the ion that gives its name to the cycle is a feedback inhibitor of citrate synthase and also inhibits PFK providing a direct link between the regulation of the citric acid cycle and glycolysis 18 Beta oxidation Edit Main article Beta oxidation In the presence of air and various cofactors and enzymes fatty acids are converted to acetyl CoA The pathway is called beta oxidation Each cycle of beta oxidation shortens the fatty acid chain by two carbon atoms and produces one equivalent each of acetyl CoA NADH and FADH2 The acetyl CoA is metabolized by the citric acid cycle to generate ATP while the NADH and FADH2 are used by oxidative phosphorylation to generate ATP Dozens of ATP equivalents are generated by the beta oxidation of a single long acyl chain 22 Regulation Edit In oxidative phosphorylation the key control point is the reaction catalyzed by cytochrome c oxidase which is regulated by the availability of its substrate the reduced form of cytochrome c The amount of reduced cytochrome c available is directly related to the amounts of other substrates 1 2 NADH cyt c ox ADP P i 1 2 NAD cyt c red ATP displaystyle frac 1 2 ce NADH ce cyt ce c ox ce ADP ce P i rightleftharpoons frac 1 2 ce NAD ce cyt ce c red ce ATP which directly implies this equation c y t c r e d c y t c o x N A D H N A D 1 2 A D P P i A T P K e q displaystyle frac mathrm cyt c red mathrm cyt c ox left frac mathrm NADH mathrm NAD right frac 1 2 left frac mathrm ADP mathrm P i mathrm ATP right K mathrm eq Thus a high ratio of NADH to NAD or a high ratio of ADP Pi to ATP imply a high amount of reduced cytochrome c and a high level of cytochrome c oxidase activity 18 An additional level of regulation is introduced by the transport rates of ATP and NADH between the mitochondrial matrix and the cytoplasm 21 Ketosis Edit Main article Ketone bodies Ketone bodies can be used as fuels yielding 22 ATP and 2 GTP molecules per acetoacetate molecule when oxidized in the mitochondria Ketone bodies are transported from the liver to other tissues where acetoacetate and beta hydroxybutyrate can be reconverted to acetyl CoA to produce reducing equivalents NADH and FADH2 via the citric acid cycle Ketone bodies cannot be used as fuel by the liver because the liver lacks the enzyme b ketoacyl CoA transferase also called thiolase Acetoacetate in low concentrations is taken up by the liver and undergoes detoxification through the methylglyoxal pathway which ends with lactate Acetoacetate in high concentrations is absorbed by cells other than those in the liver and enters a different pathway via 1 2 propanediol Though the pathway follows a different series of steps requiring ATP 1 2 propanediol can be turned into pyruvate 23 Production anaerobic conditions Edit Fermentation is the metabolism of organic compounds in the absence of air It involves substrate level phosphorylation in the absence of a respiratory electron transport chain The equation for the reaction of glucose to form lactic acid is C6 H12 O6 2 ADP 2 Pi 2 CH3 CH OH COOH 2 ATP 2 H2 OAnaerobic respiration is respiration in the absence of O2 Prokaryotes can utilize a variety of electron acceptors These include nitrate sulfate and carbon dioxide ATP replenishment by nucleoside diphosphate kinases Edit ATP can also be synthesized through several so called replenishment reactions catalyzed by the enzyme families of nucleoside diphosphate kinases NDKs which use other nucleoside triphosphates as a high energy phosphate donor and the ATP guanido phosphotransferase family ATP production during photosynthesis Edit In plants ATP is synthesized in the thylakoid membrane of the chloroplast The process is called photophosphorylation The machinery is similar to that in mitochondria except that light energy is used to pump protons across a membrane to produce a proton motive force ATP synthase then ensues exactly as in oxidative phosphorylation 24 Some of the ATP produced in the chloroplasts is consumed in the Calvin cycle which produces triose sugars ATP recycling Edit The total quantity of ATP in the human body is about 0 1 mol L 25 The majority of ATP is recycled from ADP by the aforementioned processes Thus at any given time the total amount of ATP ADP remains fairly constant The energy used by human cells in an adult requires the hydrolysis of 100 to 150 mol L of ATP daily which means a human will typically use their body weight worth of ATP over the course of the day 26 Each equivalent of ATP is recycled 1000 1500 times during a single day 150 0 1 1500 25 at approximately 9 1020 molecules s 25 An example of the Rossmann fold a structural domain of a decarboxylase enzyme from the bacterium Staphylococcus epidermidis PDB 1G5Q with a bound flavin mononucleotide cofactor Biochemical functions EditIntracellular signaling Edit ATP is involved in signal transduction by serving as substrate for kinases enzymes that transfer phosphate groups Kinases are the most common ATP binding proteins They share a small number of common folds 27 Phosphorylation of a protein by a kinase can activate a cascade such as the mitogen activated protein kinase cascade 28 ATP is also a substrate of adenylate cyclase most commonly in G protein coupled receptor signal transduction pathways and is transformed to second messenger cyclic AMP which is involved in triggering calcium signals by the release of calcium from intracellular stores 29 This form of signal transduction is particularly important in brain function although it is involved in the regulation of a multitude of other cellular processes 30 DNA and RNA synthesis Edit ATP is one of four monomers required in the synthesis of RNA The process is promoted by RNA polymerases 31 A similar process occurs in the formation of DNA except that ATP is first converted to the deoxyribonucleotide dATP Like many condensation reactions in nature DNA replication and DNA transcription also consume ATP Amino acid activation in protein synthesis Edit Main article Amino acid activation Aminoacyl tRNA synthetase enzymes consume ATP in the attachment tRNA to amino acids forming aminoacyl tRNA complexes Aminoacyl transferase binds AMP amino acid to tRNA The coupling reaction proceeds in two steps aa ATP aa AMP PPi aa AMP tRNA aa tRNA AMPThe amino acid is coupled to the penultimate nucleotide at the 3 end of the tRNA the A in the sequence CCA via an ester bond roll over in illustration ATP binding cassette transporter Edit Transporting chemicals out of a cell against a gradient is often associated with ATP hydrolysis Transport is mediated by ATP binding cassette transporters The human genome encodes 48 ABC transporters that are used for exporting drugs lipids and other compounds 32 Extracellular signalling and neurotransmission Edit Cells secrete ATP to communicate with other cells in a process called purinergic signalling ATP serves as a neurotransmitter in many parts of the nervous system modulates ciliary beating affects vascular oxygen supply etc ATP is either secreted directly across the cell membrane through channel proteins 33 34 or is pumped into vesicles 35 which then fuse with the membrane Cells detect ATP using the purinergic receptor proteins P2X and P2Y Protein solubility Edit ATP has recently been proposed to act as a biological hydrotrope 36 and has been shown to affect proteome wide solubility 37 ATP analogues EditBiochemistry laboratories often use in vitro studies to explore ATP dependent molecular processes ATP analogs are also used in X ray crystallography to determine a protein structure in complex with ATP often together with other substrates Enzyme inhibitors of ATP dependent enzymes such as kinases are needed to examine the binding sites and transition states involved in ATP dependent reactions Most useful ATP analogs cannot be hydrolyzed as ATP would be instead they trap the enzyme in a structure closely related to the ATP bound state Adenosine 5 g thiotriphosphate is an extremely common ATP analog in which one of the gamma phosphate oxygens is replaced by a sulfur atom this anion is hydrolyzed at a dramatically slower rate than ATP itself and functions as an inhibitor of ATP dependent processes In crystallographic studies hydrolysis transition states are modeled by the bound vanadate ion Caution is warranted in interpreting the results of experiments using ATP analogs since some enzymes can hydrolyze them at appreciable rates at high concentration 38 Medical use EditATP is used intravenously for some heart related conditions 39 History EditATP was discovered in 1929 by Karl Lohmann 40 and Jendrassik 41 and independently by Cyrus Fiske and Yellapragada Subba Rao of Harvard Medical School 42 both teams competing against each other to find an assay for phosphorus It was proposed to be the intermediary between energy yielding and energy requiring reactions in cells by Fritz Albert Lipmann in 1941 43 It was first synthesized in the laboratory by Alexander Todd in 1948 44 and he was awarded the Nobel Prize in Chemistry in 1957 partly for this work The 1978 Nobel Prize in Chemistry was awarded to Dr Peter Dennis Mitchell for the discovery of the 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Metabolic generation and utilization of phosphate bond energy Adv Enzymol 1 99 162 ISSN 0196 7398 History ATP first discovered in 1929 The Nobel Prize in Chemistry 1997 Nobel Foundation Archived from the original on 2010 01 23 Retrieved 2010 05 26 The Nobel Prize in Chemistry 1997 www nobelprize org Archived from the original on 24 October 2017 Retrieved 21 January 2018 External links Edit Wikimedia Commons has media related to Adenosine triphosphate ATP bound to proteins in the PDB ScienceAid Energy ATP and Exercise PubChem entry for Adenosine Triphosphate KEGG entry for Adenosine Triphosphate Retrieved from https en wikipedia org w index php title Adenosine triphosphate amp oldid 1134568273, wikipedia, wiki, book, books, library,

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