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Pyridoxal phosphate

February 15, 2024

Pyridoxal phosphate (PLP, pyridoxal 5'-phosphate, P5P), the active form of vitamin B6, is a coenzyme in a variety of enzymatic reactions. The International Union of Biochemistry and Molecular Biology has catalogued more than 140 PLP-dependent activities, corresponding to ~4% of all classified activities.[5] The versatility of PLP arises from its ability to covalently bind the substrate, and then to act as an electrophilic catalyst, thereby stabilizing different types of carbanionic reaction intermediates.

Pyridoxal phosphate


Ball-and-stick model based on the crystal structure.[1][2] Note that the phosphate and pyridine groups have reacted to form a zwitterion and the aldehyde group is hydrated.
Names
Preferred IUPAC name
(4-Formyl-5-hydroxy-6-methylpyridin-3-yl)methyl dihydrogen phosphate
Other names
Pyridoxal 5-phosphate, PAL-P, PLP, Vitamin B6 phosphate
Identifiers
  • 54-47-7 Y
3D model (JSmol)
  • Interactive image
ChEBI
  • CHEBI:18405
ChEMBL
  • ChEMBL82202 N
ECHA InfoCard 100.000.190
  • 5249
MeSH Pyridoxal+Phosphate
  • 1051
UNII
  • F06SGE49M6 Y
  • DTXSID4048351
  • O=Cc1c(O)c(C)ncc1COP(O)(O)=O
Properties
C8H10NO6P
Molar mass 247.142 g/mol
Density 1.638±0.06 g/cm3[3]
Melting point 139 to 142 °C (282 to 288 °F; 412 to 415 K)[4]
Acidity (pKa) 1.56[3]
Pharmacology
A11HA06 (WHO)
Hazards
Flash point 296.0±32.9 °C[3]
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa).
N verify (what is YN ?)

Role as a coenzyme edit

PLP acts as a coenzyme in all transamination reactions, and in certain decarboxylation, deamination, and racemization reactions of amino acids.[6] The aldehyde group of PLP forms a Schiff-base linkage (internal aldimine) with the ε-amino group of a specific lysine group of the aminotransferase enzyme. The α-amino group of the amino acid substrate displaces the ε-amino group of the active-site lysine residue in a process known as transaldimination. The resulting external aldimine can lose a proton, carbon dioxide, or an amino acid sidechain to become a quinonoid intermediate, which in turn can act as a nucleophile in several reaction pathways.

In transamination, after deprotonation the quinonoid intermediate accepts a proton at a different position to become a ketimine. The resulting ketimine is hydrolysed so that the amino group remains on the complex.[7] In addition, PLP is used by aminotransferases (or transaminases) that act upon unusual sugars such as perosamine and desosamine.[8] In these reactions, the PLP reacts with glutamate, which transfers its alpha-amino group to PLP to make pyridoxamine phosphate (PMP). PMP then transfers its nitrogen to the sugar, making an amino sugar.

PLP is also involved in various beta-elimination reactions such as the reactions carried out by serine dehydratase and GDP-4-keto-6-deoxymannose-3-dehydratase (ColD).[8]

It is also active in the condensation reaction in heme synthesis.

PLP plays a role in the conversion of levodopa into dopamine, facilitates the conversion of the excitatory neurotransmitter glutamate to the inhibitory neurotransmitter GABA, and allows SAM to be decarboxylated to form propylamine, which is a precursor to polyamines.

Role in human body edit

Main article: Vitamin B6

Pyridoxal phosphate has numerous roles in human body. A few examples below:

  • Metabolism and biosynthesis of serotonin. Pyridoxal phosphate is a cofactor of aromatic L-amino acids decarboxylase. This allows for conversion of 5-hydroxytryptophan (5-HTP) into serotonine (5-HT). This reaction takes place in serotonergic neurons.
  • Metabolism and biosynthesis of histamine. Pyridoxal phosphate is a cofactor of L-histidine decarboxylase. This allows for conversion of histidine into histamine. This reaction takes place in Golgi apparatus in mast cells and in basophils. Next, histamine is stored in granularity in mast cells as a complex with acid residues of heparin proteoglycan while in basophils as a complex with chondroitine sulfate.
  • Metabolism and biosynthesis of GABA (γ-aminobutyric acid). Pyridoxal phosphate is a cofactor of glutamic acid decarboxylase (GAD). This allows for conversion of glutamate into GABA. Reaction takes place in cytoplasm of termination of GABA-ergic neurons, therefore vitamin B6 deficiency may cause epileptic seizures in children. Pyridoxal phosphate also participates in the oxidative deamination of GABA, where it is a cofactor of GABA aminotransferase.
  • Metabolism of ornithine. Pyridoxal phosphate is a cofactor of ornithine carboxylase.
  • Transamination. Pyridoxal phosphate takes part in decomposition and synthesis of amino acids, fats, and carbohydrates, and in the biosynthesis of hormones, neurotransmitters, and heme.[9][10]

Non-classical examples of PLP edit

PLP is also found on glycogen phosphorylase in the liver, where it is used to break down glycogen in glycogenolysis when glucagon or epinephrine signals it to do so. However, this enzyme does not exploit the reactive aldehyde group, but instead utilizes the phosphate group on PLP to perform its reaction.

Although the vast majority of PLP-dependent enzymes form an internal aldimine with PLP via an active site lysine residue, some PLP-dependent enzymes do not have this lysine residue, but instead have a histidine in the active site. In such a case, the histidine cannot form the internal aldimine, and, therefore, the co-factor does not become covalently tethered to the enzyme. GDP-4-keto-6-deoxymannose-3-dehydratase (ColD) is an example of such an enzyme.[11] Human Serine hydroxymethyltransferase 2 regulates one-carbon transfer reactions required for amino acid and nucleotide metabolism, and exists in dimeric and tetrameric forms. The dimeric SHMT2 variant is a potent inhibitor of the BRISC deubiquitylase enzyme complex, which regulates immune-based cell signaling. Recent studies show that SJMT2 tetramerization is induced by PLP. This prevents interaction with the BRISC deubiqutylase complex, potentially linking vitamin B6 levels and metabolism to inflammation.[12]

Catalytic mechanism edit

The pyridoxal-5′-phosphate-dependent enzymes (PLP enzymes) catalyze myriad reactions. Although the scope of PLP-catalyzed reactions appears to be immense, the unifying principle is the formation of an internal lysine-derived aldimine. Once the amino substrate interacts with the active site, a new Schiff base is generated, commonly referred to as the external aldimine. After this step, the pathway for each PLP-catalyzed reactions diverge.[13]

 
Mechanistic examples: racemization of alanine and elimination of cysteine.

Specificity edit

Specificity is conferred by the fact that, of the four bonds of the alpha-carbon of the amino acid aldimine state, the bond perpendicular to the pyridine ring will be broken (Dunathan Stereoelectronic Hypothesis).[14][15] Consequently, specificity is dictated by how the enzymes bind their substrates. An additional role in specificity is played by the ease of protonation of the pyridine ring nitrogen.[16]

PLP-enzymes edit

PLP is retained in the active site not only thanks to the lysine, but also thanks to the interaction of the phosphate group and a phosphate binding pocket and to a lesser extent thanks to base stacking of the pyridine ring with an overhanging aromatic residue, generally tyrosine (which may also partake in the acid–base catalysis). Despite the limited requirements for a PLP binding pocket, PLP enzymes belong to only five different families. These families do not correlate well with a particular type of reaction. The five families are classified as fold types followed by a Roman numeral.[14]

  • Fold Type I — aspartate aminotransferase family
  • Fold Type II — tryptophan synthase family
  • Fold Type III — alanine racemase family (TIM-barrel)
  • Fold Type IV — D-amino acid aminotransferase family
  • Fold Type V — glycogen phosphorylase family

Biosynthesis edit

From vitamers edit

Animals are auxotroph for this enzyme co-factor and require it or an intermediate to be supplemented, hence its classification as a vitamin B6, unlike MoCo or CoQ10 for example. PLP is synthesized from pyridoxal by the enzyme pyridoxal kinase, requiring one ATP molecule. PLP is metabolized in the liver.

Prototrophy edit

Two natural pathways for PLP are currently known: one requires deoxyxylulose 5-phosphate (DXP), while the other does not, hence they are known as DXP-dependent and DXP-independent. These pathways have been studied extensively in Escherichia coli and Bacillus subtilis, respectively. Despite the disparity in the starting compounds and the different number of steps required, the two pathways possess many commonalities.[17]

DXP-dependent biosynthesis edit

The DXP-dependent biosynthetic route requires several steps and a convergence of two branches, one producing 3-hydroxy-1-aminoacetone phosphate from erythrose 4-phosphate, while the other (single enzyme) producing deoxyxylulose 5-phosphate (DXP) from glyceraldehyde 3-phosphate (GAP) and pyruvate. The condensation product of 3-hydroxy-1-aminoacetone phosphate and deoxyxylulose 5-phosphate is pyridoxine 5'-phosphate. The condensation is catalyzed by PNP synthase, encoded by pdxJ, which creates PNP (pyridoxine 5' phosphate).[18] The final enzyme is PNP oxidase (pdxH), which catalyzes the oxidation of the 4' hydroxyl group to an aldehyde using dioxigen, resulting in hydrogen peroxide.

The first branch is catalyzed in E. coli by enzymes encoded by epd, pdxB, serC and pdxA. These share mechanistical similarities and homology with the three enzymes in serine biosynthesis (serA (homologue of pdxB), serC, serB — however, epd is a homologue of gap), which points towards a shared evolutionary origin of the two pathways.[19] In several species there are two homologues of the E. coli serC gene, generally one in a ser operon (serC), and the other in a pdx operon, in which case it is called pdxF.

 

A "serendipitous pathway" was found in an overexpression library that could suppress the auxotrophy caused by the deletion of pdxB (encoding erythronate 4 phosphate dehydrogenase) in E. coli. The serendipitous pathway was very inefficient, but was possible due to the promiscuous activity of various enzymes. It started with 3-phosphohydroxypyruvate (the product of the serA-encoded enzyme in serine biosynthesis) and did not require erythronate-4-phosphate. 3PHP was dephosphorylated, resulting in an unstable intermediate that decarboxylates spontaneously (hence the presence of the phosphate in the serine biosynthetic pathway) to glycaldehyde. Glycaldehyde was condensed with glycine and the phosphorylated product was 4-phosphohydroxythreonine (4PHT), the canonical substate for 4-PHT dehydrogenase (pdxA).[20]

DXP-independent biosynthesis edit

The DXP-independent PLP-biosynthetic route consists of a step catalyzed by PLP-synthase, an enzyme composed of two subunits. PdxS catalyzes the condensation of ribulose 5-phosphate, glyceraldehyde-3-phosphate, and ammonia, this latter molecules is produced by PdxT which catalyzes the production of ammonia from glutamine. PdxS is a (β/α)8 barrel (also known as a TIM-barrel) that forms a dodecamer.[21]

Abiotic synthesis edit

The widespread utilization of PLP in central metabolism, especially in amino acid biosynthesis, and its activity in the absence of enzymes, suggests PLP may be a "prebiotic" compound—that is, one that predates the origin of organic life (not to be confused with prebiotic compounds, substances which serve as a food source for beneficial bacteria).[22] In fact, heating NH3 and Glycolaldehyde spontaneously forms a variety of pyridines, including pyridoxal.[22] Under certain conditions, PLP is formed from cyanoacetylene, diacetylene, carbon monoxide, hydrogen, water, and a phosphoric acid.[23]

Inhibitors edit

Several inhibitors of PLP enzymes are known.

One type of inhibitor forms an electrophile with PLP, causing it to irreversibly react with the active site lysine. Acetylenic compounds (e.g. propargylglycine) and vinylic compounds (e.g. vinylglycine) are such inhibitors. A different type of inhibitor inactivates PLP, and such are α-methyl and amino-oxy substrate analogs (e.g. α-methylglutamate). Still other inhibitors have good leaving groups that nucleophilically attack the PLP. Such is chloroalanine, which inhibits a large number of enzymes.[14]

Examples of inhibitors:

  • Levothyroxine In rats given only 10 µg of D, L-thyroxine daily for 15 days, liver cysteine desulfhydrase activity disappears and serine and threonine dehydrase and alanine glutamate transaminase activities decrease about 40%. Either in vivo feeding of pyridoxal-5-phosphate or in vitro addition of the coenzyme to the liver preparations restores full activity to all these enzymes, and the slight in vitro inhibition in the presence of 10−5 M thyroxine is also reversed by pyridoxal-5-phosphate.[24][25]
  • The inactive form pyridoxine competitively inhibits the active pyridoxal-5'-phosphate. Consequently, symptoms of vitamin B6 supplementation in the pyridoxine form can mimic those of vitamin B6 deficiency; an effect which perhaps might be avoided by supplementing with P5P instead.[26]
  • AlaP (alanine phosphonate) inhibits alanine racemases, but its lack of specificity has prompted further designs of ALR inhibitors.[27]
  • Gabaculine and Vigabatrin inhibit GABA aminotransferase
  • Canaline and 5-fluoromethylornithine inhibit ornithine aminotransferase
  • Amino-oxy SAM inhibits ACC synthase

Evolution edit

Pyridoxal-5-phosphate (vitamin B6)-dependent enzymes have multiple evolutionary origins. The overall B6 enzymes diverged into four independent evolutionary lines: α family (i.e. aspartate aminotransferase), β family (serine dehydratase),D-alanine aminotransferase family and the alanine racemase family. An example of the evolutionary similarity in the Beta family is seen in the mechanism. The β enzymes are all lyases and catalyze reactions where Cα and Cβ participate. Overall, in the PLP-dependent enzymes, the PLP in every case is covalently attached via an imine bond to the amino group in the active site.[28]

See also edit

References edit

  1. ^ "CSD Entry: PLPHYD10". Cambridge Structural Database: Access Structures. Cambridge Crystallographic Data Centre. 1974. Retrieved 2023-11-04.
  2. ^ Fujiwara T (1973). "The Crystal and Molecular Structure of Vitamin B6 Derivatives. I. Pyridoxal Phosphate Hydrate and Pyridoxal Phosphate Methyl Hemiacetal". Bull. Chem. Soc. Jpn. 46 (3): 863–871. doi:10.1246/bcsj.46.863.
  3. ^ a b c Calculated using Advanced Chemistry Development (ACD/Labs) Software V11.02 (© 1994-2011 ACD/Labs)
  4. ^ Kozlov ÉI, L'vova MS (1978). "Stability of water-soluble vitamins and coenzymes. Hydrolysis of pyridoxal-5-phosphate in acidic, neutral, and weakly alkaline solutions". Pharmaceutical Chemistry Journal. 11 (11): 1543–9. doi:10.1007/BF00778244. S2CID 1094223.
  5. ^ Percudani R, Peracchi A (September 2003). "A genomic overview of pyridoxal-phosphate-dependent enzymes". EMBO Reports. 4 (9): 850–4. doi:10.1038/sj.embor.embor914. PMC 1326353. PMID 12949584.
  6. ^ Dolphin D, Poulson R, Avramovic O (1986). "Vitamin B6: Pyridoxal Phosphate" (PDF). Coenzymes and Cofactors. Vol. 1, Part B. New York: Wiley Interscience. ISBN 978-0471097853.
  7. ^ Toney MD (January 2005). "Reaction specificity in pyridoxal phosphate enzymes". Archives of Biochemistry and Biophysics. 433 (1): 279–87. doi:10.1016/j.abb.2004.09.037. PMID 15581583.
  8. ^ a b Samuel G, Reeves P (November 2003). "Biosynthesis of O-antigens: genes and pathways involved in nucleotide sugar precursor synthesis and O-antigen assembly". Carbohydrate Research. 338 (23): 2503–19. doi:10.1016/j.carres.2003.07.009. PMID 14670712.
  9. ^ Lutz MB, Romani N, Steinkasserer A, eds. (2006-02-06). Handbook of Dendritic Cells: Biology, Diseases, and Therapies (1 ed.). Wiley. doi:10.1002/9783527619696. ISBN 978-3-527-31109-5. S2CID 183733461.
  10. ^ Rucker RB, ed. (2001). Handbook of vitamins. Clinical nutrition in health and disease (3. ed., rev. and expanded ed.). New York, NY: Dekker. ISBN 978-0-8247-0428-5.
  11. ^ Cook PD, Thoden JB, Holden HM (September 2006). "The structure of GDP-4-keto-6-deoxy-D-mannose-3-dehydratase: a unique coenzyme B6-dependent enzyme". Protein Science. 15 (9): 2093–106. doi:10.1110/ps.062328306. PMC 2242600. PMID 16943443.
  12. ^ Eyers PA, Murphy JM (November 2016). "The evolving world of pseudoenzymes: proteins, prejudice and zombies". BMC Biology. 14 (1): 98. doi:10.1186/s12915-016-0322-x. PMC 5106787. PMID 27835992.
  13. ^ Eliot AC, Kirsch JF (2004). "Pyridoxal Phosphate Enzymes: Mechanistic, Structural, and Evolutionary Considerations". Annual Review of Biochemistry. 73: 383–415. doi:10.1146/annurev.biochem.73.011303.074021. PMID 15189147.
  14. ^ a b c Eliot AC, Kirsch JF (2004). "Pyridoxal phosphate enzymes: mechanistic, structural, and evolutionary considerations". Annual Review of Biochemistry. 73: 383–415. doi:10.1146/annurev.biochem.73.011303.074021. PMID 15189147. S2CID 36010634.
  15. ^ Gayathri SC, Manoj N (December 2020). "Crystallographic Snapshots of the Dunathan and Quinonoid Intermediates provide Insights into the Reaction Mechanism of Group II Decarboxylases". Journal of Molecular Biology. 432 (24): 166692. doi:10.1016/j.jmb.2020.10.026. PMID 33122004. S2CID 226205717.
  16. ^ Griswold WR, Toney MD (September 2011). "Role of the pyridine nitrogen in pyridoxal 5'-phosphate catalysis: activity of three classes of PLP enzymes reconstituted with deazapyridoxal 5'-phosphate". Journal of the American Chemical Society. 133 (37): 14823–30. doi:10.1021/ja2061006. PMID 21827189. S2CID 10780336.
  17. ^ Fitzpatrick TB, Amrhein N, Kappes B, Macheroux P, Tews I, Raschle T (October 2007). "Two independent routes of de novo vitamin B6 biosynthesis: not that different after all". The Biochemical Journal. 407 (1): 1–13. doi:10.1042/BJ20070765. PMC 2267407. PMID 17822383. S2CID 28231094.
  18. ^ Sakai A, Kita M, Tani Y (April 2004). "Recent progress of vitamin B6 biosynthesis". Journal of Nutritional Science and Vitaminology. 50 (2): 69–77. doi:10.3177/jnsv.50.69. PMID 15242009.
  19. ^ Lam HM, Winkler ME (November 1990). "Metabolic relationships between pyridoxine (vitamin B6) and serine biosynthesis in Escherichia coli K-12". Journal of Bacteriology. 172 (11): 6518–28. doi:10.1128/jb.172.11.6518-6528.1990. PMC 526841. PMID 2121717.
  20. ^ Kim J, Kershner JP, Novikov Y, Shoemaker RK, Copley SD (November 2010). "Three serendipitous pathways in E. coli can bypass a block in pyridoxal-5'-phosphate synthesis". Molecular Systems Biology. 6: 436. doi:10.1038/msb.2010.88. PMC 3010111. PMID 21119630.
  21. ^ Zhu J, Burgner JW, Harms E, Belitsky BR, Smith JL (July 2005). "A new arrangement of (beta/alpha)8 barrels in the synthase subunit of PLP synthase". The Journal of Biological Chemistry. 280 (30): 27914–23. doi:10.1074/jbc.M503642200. PMID 15911615.
  22. ^ a b Austin SM, Waddell TG (May 1999). "Prebiotic synthesis of vitamin B6-type compounds". Origins of Life and Evolution of the Biosphere. 29 (3): 287–96. Bibcode:1999OLEB...29..287A. doi:10.1023/A:1006532518221. PMID 10389266. S2CID 22284565.
  23. ^ Aylward N, Bofinger N (September 2006). "A plausible prebiotic synthesis of pyridoxal phosphate: vitamin B6 - a computational study". Biophysical Chemistry. 123 (2–3): 113–21. doi:10.1016/j.bpc.2006.04.014. PMID 16730878.
  24. ^ Horvath A (1957). "Inhibition by Thyroxine of Enzymes requiring Pyridoxal-5-Phosphate". Nature. 179 (4567): 968. Bibcode:1957Natur.179..968H. doi:10.1038/179968a0. PMID 13430754. S2CID 4262396.
  25. ^ Hoch FL (1962). "Biochemical Actions of Thyroid Hormones". Physiological Reviews. 42 (4): 605–673. doi:10.1152/physrev.1962.42.4.605. PMID 13954890.
  26. ^ Vrolijk MF, Opperhuizen A, Jansen EH, Hageman GJ, Bast A, Haenen GR (2017). "The vitamin B6 paradox: Supplementation with high concentrations of pyridoxine leads to decreased vitamin B6 function". Toxicology in Vitro. 44: 206–212. doi:10.1016/j.tiv.2017.07.009. PMID 28716455.
  27. ^ Anthony KG, Strych U, Yeung KR, Shoen CS, Perez O, Krause KL, et al. (2011). Ahmed N (ed.). "New classes of alanine racemase inhibitors identified by high-throughput screening show antimicrobial activity against Mycobacterium tuberculosis". PLOS ONE. 6 (5): e20374. Bibcode:2011PLoSO...620374A. doi:10.1371/journal.pone.0020374. PMC 3102704. PMID 21637807.
  28. ^ Christen P, Mehta PK (2001). "From cofactor to enzymes. The molecular evolution of pyridoxal-5'-phosphate-dependent enzymes". Chemical Record. 1 (6): 436–47. doi:10.1002/tcr.10005. PMID 11933250.

External links edit

February 15, 2024
pyridoxal, phosphate, pyridoxal, phosphate, active, form, vitamin, coenzyme, variety, enzymatic, reactions, international, union, biochemistry, molecular, biology, catalogued, more, than, dependent, activities, corresponding, classified, activities, versatilit. Pyridoxal phosphate PLP pyridoxal 5 phosphate P5P the active form of vitamin B6 is a coenzyme in a variety of enzymatic reactions The International Union of Biochemistry and Molecular Biology has catalogued more than 140 PLP dependent activities corresponding to 4 of all classified activities 5 The versatility of PLP arises from its ability to covalently bind the substrate and then to act as an electrophilic catalyst thereby stabilizing different types of carbanionic reaction intermediates Pyridoxal phosphate Idealised skeletal formulaBall and stick model based on the crystal structure 1 2 Note that the phosphate and pyridine groups have reacted to form a zwitterion and the aldehyde group is hydrated NamesPreferred IUPAC name 4 Formyl 5 hydroxy 6 methylpyridin 3 yl methyl dihydrogen phosphateOther names Pyridoxal 5 phosphate PAL P PLP Vitamin B6 phosphateIdentifiersCAS Number 54 47 7 Y3D model JSmol Interactive imageChEBI CHEBI 18405ChEMBL ChEMBL82202 NECHA InfoCard 100 000 190IUPHAR BPS 5249MeSH Pyridoxal PhosphatePubChem CID 1051UNII F06SGE49M6 YCompTox Dashboard EPA DTXSID4048351SMILES O Cc1c O c C ncc1COP O O OPropertiesChemical formula C8H10NO6PMolar mass 247 142 g molDensity 1 638 0 06 g cm3 3 Melting point 139 to 142 C 282 to 288 F 412 to 415 K 4 Acidity pKa 1 56 3 PharmacologyATC code A11HA06 WHO HazardsFlash point 296 0 32 9 C 3 Except where otherwise noted data are given for materials in their standard state at 25 C 77 F 100 kPa N verify what is Y N Infobox references Contents 1 Role as a coenzyme 2 Role in human body 3 Non classical examples of PLP 4 Catalytic mechanism 5 Specificity 6 PLP enzymes 7 Biosynthesis 7 1 From vitamers 7 2 Prototrophy 7 2 1 DXP dependent biosynthesis 7 2 2 DXP independent biosynthesis 7 3 Abiotic synthesis 8 Inhibitors 9 Evolution 10 See also 11 References 12 External linksRole as a coenzyme editPLP acts as a coenzyme in all transamination reactions and in certain decarboxylation deamination and racemization reactions of amino acids 6 The aldehyde group of PLP forms a Schiff base linkage internal aldimine with the e amino group of a specific lysine group of the aminotransferase enzyme The a amino group of the amino acid substrate displaces the e amino group of the active site lysine residue in a process known as transaldimination The resulting external aldimine can lose a proton carbon dioxide or an amino acid sidechain to become a quinonoid intermediate which in turn can act as a nucleophile in several reaction pathways In transamination after deprotonation the quinonoid intermediate accepts a proton at a different position to become a ketimine The resulting ketimine is hydrolysed so that the amino group remains on the complex 7 In addition PLP is used by aminotransferases or transaminases that act upon unusual sugars such as perosamine and desosamine 8 In these reactions the PLP reacts with glutamate which transfers its alpha amino group to PLP to make pyridoxamine phosphate PMP PMP then transfers its nitrogen to the sugar making an amino sugar PLP is also involved in various beta elimination reactions such as the reactions carried out by serine dehydratase and GDP 4 keto 6 deoxymannose 3 dehydratase ColD 8 It is also active in the condensation reaction in heme synthesis PLP plays a role in the conversion of levodopa into dopamine facilitates the conversion of the excitatory neurotransmitter glutamate to the inhibitory neurotransmitter GABA and allows SAM to be decarboxylated to form propylamine which is a precursor to polyamines Role in human body editMain article Vitamin B6 Pyridoxal phosphate has numerous roles in human body A few examples below Metabolism and biosynthesis of serotonin Pyridoxal phosphate is a cofactor of aromatic L amino acids decarboxylase This allows for conversion of 5 hydroxytryptophan 5 HTP into serotonine 5 HT This reaction takes place in serotonergic neurons Metabolism and biosynthesis of histamine Pyridoxal phosphate is a cofactor of L histidine decarboxylase This allows for conversion of histidine into histamine This reaction takes place in Golgi apparatus in mast cells and in basophils Next histamine is stored in granularity in mast cells as a complex with acid residues of heparin proteoglycan while in basophils as a complex with chondroitine sulfate Metabolism and biosynthesis of GABA g aminobutyric acid Pyridoxal phosphate is a cofactor of glutamic acid decarboxylase GAD This allows for conversion of glutamate into GABA Reaction takes place in cytoplasm of termination of GABA ergic neurons therefore vitamin B6 deficiency may cause epileptic seizures in children Pyridoxal phosphate also participates in the oxidative deamination of GABA where it is a cofactor of GABA aminotransferase Metabolism of ornithine Pyridoxal phosphate is a cofactor of ornithine carboxylase Transamination Pyridoxal phosphate takes part in decomposition and synthesis of amino acids fats and carbohydrates and in the biosynthesis of hormones neurotransmitters and heme 9 10 Non classical examples of PLP editPLP is also found on glycogen phosphorylase in the liver where it is used to break down glycogen in glycogenolysis when glucagon or epinephrine signals it to do so However this enzyme does not exploit the reactive aldehyde group but instead utilizes the phosphate group on PLP to perform its reaction Although the vast majority of PLP dependent enzymes form an internal aldimine with PLP via an active site lysine residue some PLP dependent enzymes do not have this lysine residue but instead have a histidine in the active site In such a case the histidine cannot form the internal aldimine and therefore the co factor does not become covalently tethered to the enzyme GDP 4 keto 6 deoxymannose 3 dehydratase ColD is an example of such an enzyme 11 Human Serine hydroxymethyltransferase 2 regulates one carbon transfer reactions required for amino acid and nucleotide metabolism and exists in dimeric and tetrameric forms The dimeric SHMT2 variant is a potent inhibitor of the BRISC deubiquitylase enzyme complex which regulates immune based cell signaling Recent studies show that SJMT2 tetramerization is induced by PLP This prevents interaction with the BRISC deubiqutylase complex potentially linking vitamin B6 levels and metabolism to inflammation 12 Catalytic mechanism editThe pyridoxal 5 phosphate dependent enzymes PLP enzymes catalyze myriad reactions Although the scope of PLP catalyzed reactions appears to be immense the unifying principle is the formation of an internal lysine derived aldimine Once the amino substrate interacts with the active site a new Schiff base is generated commonly referred to as the external aldimine After this step the pathway for each PLP catalyzed reactions diverge 13 nbsp Mechanistic examples racemization of alanine and elimination of cysteine Specificity editSpecificity is conferred by the fact that of the four bonds of the alpha carbon of the amino acid aldimine state the bond perpendicular to the pyridine ring will be broken Dunathan Stereoelectronic Hypothesis 14 15 Consequently specificity is dictated by how the enzymes bind their substrates An additional role in specificity is played by the ease of protonation of the pyridine ring nitrogen 16 PLP enzymes editPLP is retained in the active site not only thanks to the lysine but also thanks to the interaction of the phosphate group and a phosphate binding pocket and to a lesser extent thanks to base stacking of the pyridine ring with an overhanging aromatic residue generally tyrosine which may also partake in the acid base catalysis Despite the limited requirements for a PLP binding pocket PLP enzymes belong to only five different families These families do not correlate well with a particular type of reaction The five families are classified as fold types followed by a Roman numeral 14 Fold Type I aspartate aminotransferase family Fold Type II tryptophan synthase family Fold Type III alanine racemase family TIM barrel Fold Type IV D amino acid aminotransferase family Fold Type V glycogen phosphorylase familyBiosynthesis editFrom vitamers edit Animals are auxotroph for this enzyme co factor and require it or an intermediate to be supplemented hence its classification as a vitamin B6 unlike MoCo or CoQ10 for example PLP is synthesized from pyridoxal by the enzyme pyridoxal kinase requiring one ATP molecule PLP is metabolized in the liver Prototrophy edit Two natural pathways for PLP are currently known one requires deoxyxylulose 5 phosphate DXP while the other does not hence they are known as DXP dependent and DXP independent These pathways have been studied extensively in Escherichia coli and Bacillus subtilis respectively Despite the disparity in the starting compounds and the different number of steps required the two pathways possess many commonalities 17 DXP dependent biosynthesis edit The DXP dependent biosynthetic route requires several steps and a convergence of two branches one producing 3 hydroxy 1 aminoacetone phosphate from erythrose 4 phosphate while the other single enzyme producing deoxyxylulose 5 phosphate DXP from glyceraldehyde 3 phosphate GAP and pyruvate The condensation product of 3 hydroxy 1 aminoacetone phosphate and deoxyxylulose 5 phosphate is pyridoxine 5 phosphate The condensation is catalyzed by PNP synthase encoded by pdxJ which creates PNP pyridoxine 5 phosphate 18 The final enzyme is PNP oxidase pdxH which catalyzes the oxidation of the 4 hydroxyl group to an aldehyde using dioxigen resulting in hydrogen peroxide The first branch is catalyzed in E coli by enzymes encoded by epd pdxB serC and pdxA These share mechanistical similarities and homology with the three enzymes in serine biosynthesis serA homologue of pdxB serC serB however epd is a homologue of gap which points towards a shared evolutionary origin of the two pathways 19 In several species there are two homologues of the E coli serC gene generally one in a ser operon serC and the other in a pdx operon in which case it is called pdxF nbsp A serendipitous pathway was found in an overexpression library that could suppress the auxotrophy caused by the deletion of pdxB encoding erythronate 4 phosphate dehydrogenase in E coli The serendipitous pathway was very inefficient but was possible due to the promiscuous activity of various enzymes It started with 3 phosphohydroxypyruvate the product of the serA encoded enzyme in serine biosynthesis and did not require erythronate 4 phosphate 3PHP was dephosphorylated resulting in an unstable intermediate that decarboxylates spontaneously hence the presence of the phosphate in the serine biosynthetic pathway to glycaldehyde Glycaldehyde was condensed with glycine and the phosphorylated product was 4 phosphohydroxythreonine 4PHT the canonical substate for 4 PHT dehydrogenase pdxA 20 DXP independent biosynthesis edit The DXP independent PLP biosynthetic route consists of a step catalyzed by PLP synthase an enzyme composed of two subunits PdxS catalyzes the condensation of ribulose 5 phosphate glyceraldehyde 3 phosphate and ammonia this latter molecules is produced by PdxT which catalyzes the production of ammonia from glutamine PdxS is a b a 8 barrel also known as a TIM barrel that forms a dodecamer 21 Abiotic synthesis edit The widespread utilization of PLP in central metabolism especially in amino acid biosynthesis and its activity in the absence of enzymes suggests PLP may be a prebiotic compound that is one that predates the origin of organic life not to be confused with prebiotic compounds substances which serve as a food source for beneficial bacteria 22 In fact heating NH3 and Glycolaldehyde spontaneously forms a variety of pyridines including pyridoxal 22 Under certain conditions PLP is formed from cyanoacetylene diacetylene carbon monoxide hydrogen water and a phosphoric acid 23 Inhibitors editSeveral inhibitors of PLP enzymes are known One type of inhibitor forms an electrophile with PLP causing it to irreversibly react with the active site lysine Acetylenic compounds e g propargylglycine and vinylic compounds e g vinylglycine are such inhibitors A different type of inhibitor inactivates PLP and such are a methyl and amino oxy substrate analogs e g a methylglutamate Still other inhibitors have good leaving groups that nucleophilically attack the PLP Such is chloroalanine which inhibits a large number of enzymes 14 Examples of inhibitors Levothyroxine In rats given only 10 µg of D L thyroxine daily for 15 days liver cysteine desulfhydrase activity disappears and serine and threonine dehydrase and alanine glutamate transaminase activities decrease about 40 Either in vivo feeding of pyridoxal 5 phosphate or in vitro addition of the coenzyme to the liver preparations restores full activity to all these enzymes and the slight in vitro inhibition in the presence of 10 5 M thyroxine is also reversed by pyridoxal 5 phosphate 24 25 The inactive form pyridoxine competitively inhibits the active pyridoxal 5 phosphate Consequently symptoms of vitamin B6 supplementation in the pyridoxine form can mimic those of vitamin B6 deficiency an effect which perhaps might be avoided by supplementing with P5P instead 26 AlaP alanine phosphonate inhibits alanine racemases but its lack of specificity has prompted further designs of ALR inhibitors 27 Gabaculine and Vigabatrin inhibit GABA aminotransferase Canaline and 5 fluoromethylornithine inhibit ornithine aminotransferase Amino oxy SAM inhibits ACC synthaseEvolution editPyridoxal 5 phosphate vitamin B6 dependent enzymes have multiple evolutionary origins The overall B6 enzymes diverged into four independent evolutionary lines a family i e aspartate aminotransferase b family serine dehydratase D alanine aminotransferase family and the alanine racemase family An example of the evolutionary similarity in the Beta family is seen in the mechanism The b enzymes are all lyases and catalyze reactions where Ca and Cb participate Overall in the PLP dependent enzymes the PLP in every case is covalently attached via an imine bond to the amino group in the active site 28 See also editAromatic L amino acid decarboxylase Ornithine decarboxylaseReferences edit CSD Entry PLPHYD10 Cambridge Structural Database Access Structures Cambridge Crystallographic Data Centre 1974 Retrieved 2023 11 04 Fujiwara T 1973 The Crystal and Molecular Structure of Vitamin B6 Derivatives I Pyridoxal Phosphate Hydrate and Pyridoxal Phosphate Methyl Hemiacetal Bull Chem Soc Jpn 46 3 863 871 doi 10 1246 bcsj 46 863 a b c Calculated using Advanced Chemistry Development ACD Labs Software V11 02 c 1994 2011 ACD Labs Kozlov EI L vova MS 1978 Stability of water soluble vitamins and coenzymes Hydrolysis of pyridoxal 5 phosphate in acidic neutral and weakly alkaline solutions Pharmaceutical Chemistry Journal 11 11 1543 9 doi 10 1007 BF00778244 S2CID 1094223 Percudani R Peracchi A September 2003 A genomic overview of pyridoxal phosphate dependent enzymes EMBO Reports 4 9 850 4 doi 10 1038 sj embor embor914 PMC 1326353 PMID 12949584 Dolphin D Poulson R Avramovic O 1986 Vitamin B6 Pyridoxal Phosphate PDF Coenzymes and Cofactors Vol 1 Part B New York Wiley Interscience ISBN 978 0471097853 Toney MD January 2005 Reaction specificity in pyridoxal phosphate enzymes Archives of Biochemistry and Biophysics 433 1 279 87 doi 10 1016 j abb 2004 09 037 PMID 15581583 a b Samuel G Reeves P November 2003 Biosynthesis of O antigens genes and pathways involved in nucleotide sugar precursor synthesis and O antigen assembly Carbohydrate Research 338 23 2503 19 doi 10 1016 j carres 2003 07 009 PMID 14670712 Lutz MB Romani N Steinkasserer A eds 2006 02 06 Handbook of Dendritic Cells Biology Diseases and Therapies 1 ed Wiley doi 10 1002 9783527619696 ISBN 978 3 527 31109 5 S2CID 183733461 Rucker RB ed 2001 Handbook of vitamins Clinical nutrition in health and disease 3 ed rev and expanded ed New York NY Dekker ISBN 978 0 8247 0428 5 Cook PD Thoden JB Holden HM September 2006 The structure of GDP 4 keto 6 deoxy D mannose 3 dehydratase a unique coenzyme B6 dependent enzyme Protein Science 15 9 2093 106 doi 10 1110 ps 062328306 PMC 2242600 PMID 16943443 Eyers PA Murphy JM November 2016 The evolving world of pseudoenzymes proteins prejudice and zombies BMC Biology 14 1 98 doi 10 1186 s12915 016 0322 x PMC 5106787 PMID 27835992 Eliot AC Kirsch JF 2004 Pyridoxal Phosphate Enzymes Mechanistic Structural and Evolutionary Considerations Annual Review of Biochemistry 73 383 415 doi 10 1146 annurev biochem 73 011303 074021 PMID 15189147 a b c Eliot AC Kirsch JF 2004 Pyridoxal phosphate enzymes mechanistic structural and evolutionary considerations Annual Review of Biochemistry 73 383 415 doi 10 1146 annurev biochem 73 011303 074021 PMID 15189147 S2CID 36010634 Gayathri SC Manoj N December 2020 Crystallographic Snapshots of the Dunathan and Quinonoid Intermediates provide Insights into the Reaction Mechanism of Group II Decarboxylases Journal of Molecular Biology 432 24 166692 doi 10 1016 j jmb 2020 10 026 PMID 33122004 S2CID 226205717 Griswold WR Toney MD September 2011 Role of the pyridine nitrogen in pyridoxal 5 phosphate catalysis activity of three classes of PLP enzymes reconstituted with deazapyridoxal 5 phosphate Journal of the American Chemical Society 133 37 14823 30 doi 10 1021 ja2061006 PMID 21827189 S2CID 10780336 Fitzpatrick TB Amrhein N Kappes B Macheroux P Tews I Raschle T October 2007 Two independent routes of de novo vitamin B6 biosynthesis not that different after all The Biochemical Journal 407 1 1 13 doi 10 1042 BJ20070765 PMC 2267407 PMID 17822383 S2CID 28231094 Sakai A Kita M Tani Y April 2004 Recent progress of vitamin B6 biosynthesis Journal of Nutritional Science and Vitaminology 50 2 69 77 doi 10 3177 jnsv 50 69 PMID 15242009 Lam HM Winkler ME November 1990 Metabolic relationships between pyridoxine vitamin B6 and serine biosynthesis in Escherichia coli K 12 Journal of Bacteriology 172 11 6518 28 doi 10 1128 jb 172 11 6518 6528 1990 PMC 526841 PMID 2121717 Kim J Kershner JP Novikov Y Shoemaker RK Copley SD November 2010 Three serendipitous pathways in E coli can bypass a block in pyridoxal 5 phosphate synthesis Molecular Systems Biology 6 436 doi 10 1038 msb 2010 88 PMC 3010111 PMID 21119630 Zhu J Burgner JW Harms E Belitsky BR Smith JL July 2005 A new arrangement of beta alpha 8 barrels in the synthase subunit of PLP synthase The Journal of Biological Chemistry 280 30 27914 23 doi 10 1074 jbc M503642200 PMID 15911615 a b Austin SM Waddell TG May 1999 Prebiotic synthesis of vitamin B6 type compounds Origins of Life and Evolution of the Biosphere 29 3 287 96 Bibcode 1999OLEB 29 287A doi 10 1023 A 1006532518221 PMID 10389266 S2CID 22284565 Aylward N Bofinger N September 2006 A plausible prebiotic synthesis of pyridoxal phosphate vitamin B6 a computational study Biophysical Chemistry 123 2 3 113 21 doi 10 1016 j bpc 2006 04 014 PMID 16730878 Horvath A 1957 Inhibition by Thyroxine of Enzymes requiring Pyridoxal 5 Phosphate Nature 179 4567 968 Bibcode 1957Natur 179 968H doi 10 1038 179968a0 PMID 13430754 S2CID 4262396 Hoch FL 1962 Biochemical Actions of Thyroid Hormones Physiological Reviews 42 4 605 673 doi 10 1152 physrev 1962 42 4 605 PMID 13954890 Vrolijk MF Opperhuizen A Jansen EH Hageman GJ Bast A Haenen GR 2017 The vitamin B6 paradox Supplementation with high concentrations of pyridoxine leads to decreased vitamin B6 function Toxicology in Vitro 44 206 212 doi 10 1016 j tiv 2017 07 009 PMID 28716455 Anthony KG Strych U Yeung KR Shoen CS Perez O Krause KL et al 2011 Ahmed N ed New classes of alanine racemase inhibitors identified by high throughput screening show antimicrobial activity against Mycobacterium tuberculosis PLOS ONE 6 5 e20374 Bibcode 2011PLoSO 620374A doi 10 1371 journal pone 0020374 PMC 3102704 PMID 21637807 Christen P Mehta PK 2001 From cofactor to enzymes The molecular evolution of pyridoxal 5 phosphate dependent enzymes Chemical Record 1 6 436 47 doi 10 1002 tcr 10005 PMID 11933250 External links editA11HA06 WHO Retrieved from https en wikipedia org w index php title Pyridoxal phosphate amp oldid 1199149380, wikipedia, wiki, book, books, library,

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