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Wikipedia

Phenylalanine

May 19, 2023

Phenylalanine (symbol Phe or F)[3] is an essential α-amino acid with the formula C
9H
11NO
2. It can be viewed as a benzyl group substituted for the methyl group of alanine, or a phenyl group in place of a terminal hydrogen of alanine. This essential amino acid is classified as neutral, and nonpolar because of the inert and hydrophobic nature of the benzyl side chain. The L-isomer is used to biochemically form proteins coded for by DNA. Phenylalanine is a precursor for tyrosine, the monoamine neurotransmitters dopamine, norepinephrine (noradrenaline), and epinephrine (adrenaline), and the skin pigment melanin. It is encoded by the codons UUU and UUC.

Phenylalanine

Skeletal formula of L-phenylalanine

L-Phenylalanine at physiological pH
Names
Pronunciation US: /ˌfɛnəlˈælənn/; UK: /ˌfnl-/
IUPAC name
Phenylalanine
Systematic IUPAC name
(S)-2-Amino-3-phenylpropanoic acid
Identifiers
  • L: 63-91-2 Y
  • D/L: 150-30-1 Y
  • D: 673-06-3 Y
3D model (JSmol)
  • L: Interactive image
  • L Zwitterion: Interactive image
ChEBI
  • L: CHEBI:17295 Y
  • D: CHEBI:16998 Y
ChEMBL
  • L: ChEMBL301523 Y
ChemSpider
  • L: 5910 Y
  • D/L: 969 Y
  • D: 64639 Y
DrugBank
  • L: DB00120 Y
ECHA InfoCard 100.000.517
  • L: 3313
KEGG
  • L: D00021 Y
  • L: 6140
  • D/L: 994
  • D: 71567
UNII
  • L: 47E5O17Y3R Y
  • D/L: 8P946UF12S Y
  • D: 032K16VRCU Y
  • L: DTXSID4040763
  • InChI=1S/C9H11NO2/c10-8(9(11)12)6-7-4-2-1-3-5-7/h1-5,8H,6,10H2,(H,11,12)/t8-/m0/s1 Y
    Key: COLNVLDHVKWLRT-QMMMGPOBSA-N Y
  • L: Key: COLNVLDHVKWLRT-QMMMGPOBBC
  • D/L: Key: COLNVLDHVKWLRT-UHFFFAOYSA-N
  • D: Key: COLNVLDHVKWLRT-MRVPVSSYSA-N
  • L: c1ccc(cc1)C[C@@H](C(=O)O)N
  • L Zwitterion: [NH3+][C@@H](CC1=CC=CC=C1)C([O-])=O
Properties
C9H11NO2
Molar mass 165.192 g·mol−1
Acidity (pKa) 1.83 (carboxyl), 9.13 (amino)[2]
Hazards
NFPA 704 (fire diamond)
2
1
0
Supplementary data page
Phenylalanine (data page)
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa).

Phenylalanine is found naturally in the milk of mammals. It is used in the manufacture of food and drink products and sold as a nutritional supplement for its analgesic and antidepressant effects. It is a direct precursor to the neuromodulator phenethylamine, a commonly used dietary supplement. As an essential amino acid, phenylalanine is not synthesized de novo in humans and other animals, who must ingest phenylalanine or phenylalanine-containing proteins.

History

The first description of phenylalanine was made in 1879, when Schulze and Barbieri identified a compound with the empirical formula, C9H11NO2, in yellow lupine (Lupinus luteus) seedlings. In 1882, Erlenmeyer and Lipp first synthesized phenylalanine from phenylacetaldehyde, hydrogen cyanide, and ammonia.[4][5]

The genetic codon for phenylalanine was first discovered by J. Heinrich Matthaei and Marshall W. Nirenberg in 1961. They showed that by using mRNA to insert multiple uracil repeats into the genome of the bacterium E. coli, they could cause the bacterium to produce a polypeptide consisting solely of repeated phenylalanine amino acids. This discovery helped to establish the nature of the coding relationship that links information stored in genomic nucleic acid with protein expression in the living cell.

Dietary sources

Good sources of phenylalanine are eggs, chicken, liver, beef, milk, and soybeans.[6] Another common source of phenylalanine is anything sweetened with the artificial sweetener aspartame, such as diet drinks, diet foods and medication; the metabolism of aspartame produces phenylalanine as one of the compound's metabolites.[7]

Dietary recommendations

The Food and Nutrition Board (FNB) of the U.S. Institute of Medicine set Recommended Dietary Allowances (RDAs) for essential amino acids in 2002. For phenylalanine plus tyrosine, for adults 19 years and older, 33 mg/kg body weight/day.[8] In 2005 the DRI is set to 27 mg/kg per day (with no tyrosine), the FAO/WHO/UNU recommendation of 2007 is 25 mg/kg per day (with no tyrosine).[9]

Other biological roles

L-Phenylalanine is biologically converted into L-tyrosine, another one of the DNA-encoded amino acids. L-tyrosine in turn is converted into L-DOPA, which is further converted into dopamine, norepinephrine (noradrenaline), and epinephrine (adrenaline). The latter three are known as the catecholamines.

Phenylalanine uses the same active transport channel as tryptophan to cross the blood–brain barrier. In excessive quantities, supplementation can interfere with the production of serotonin and other aromatic amino acids[10] as well as nitric oxide due to the overuse (eventually, limited availability) of the associated cofactors, iron or tetrahydrobiopterin.[citation needed] The corresponding enzymes for those compounds are the aromatic amino acid hydroxylase family and nitric oxide synthase.

Biosynthetic pathways for catecholamines and trace amines in the human brain[11][12][13]
 
Phenylalanine in humans may ultimately be metabolized into a range of different substances.

In plants

Phenylalanine is the starting compound used in the synthesis of flavonoids. Lignan is derived from phenylalanine and from tyrosine. Phenylalanine is converted to cinnamic acid by the enzyme phenylalanine ammonia-lyase.[14]

Biosynthesis

Phenylalanine is biosynthesized via the Shikimate pathway.

Phenylketonuria

Main article: Phenylketonuria

The genetic disorder phenylketonuria (PKU) is the inability to metabolize phenylalanine because of a lack of the enzyme phenylalanine hydroxylase. Individuals with this disorder are known as "phenylketonurics" and must regulate their intake of phenylalanine. Phenylketonurics often use blood tests to monitor the amount of phenylalanine in their blood. Lab results may report phenylalanine levels using either mg/dL and μmol/L. One mg/dL of phenylalanine is approximately equivalent to 60 μmol/L.

A (rare) "variant form" of phenylketonuria called hyperphenylalaninemia is caused by the inability to synthesize a cofactor called tetrahydrobiopterin, which can be supplemented. Pregnant women with hyperphenylalaninemia may show similar symptoms of the disorder (high levels of phenylalanine in blood), but these indicators will usually disappear at the end of gestation. Pregnant women with PKU must control their blood phenylalanine levels even if the fetus is heterozygous for the defective gene because the fetus could be adversely affected due to hepatic immaturity.[medical citation needed]

A non-food source of phenylalanine is the artificial sweetener aspartame. This compound is metabolized by the body into several chemical byproducts including phenylalanine. The breakdown problems phenylketonurics have with the buildup of phenylalanine in the body also occurs with the ingestion of aspartame, although to a lesser degree. Accordingly, all products in Australia, the U.S. and Canada that contain aspartame must be labeled: "Phenylketonurics: Contains phenylalanine." In the UK, foods containing aspartame must carry ingredient panels that refer to the presence of "aspartame or E951"[15] and they must be labeled with a warning "Contains a source of phenylalanine." In Brazil, the label "Contém Fenilalanina" (Portuguese for "Contains Phenylalanine") is also mandatory in products which contain it. These warnings are placed to help individuals avoid such foods.

D-, L- and DL-phenylalanine

The stereoisomer D-phenylalanine (DPA) can be produced by conventional organic synthesis, either as a single enantiomer or as a component of the racemic mixture. It does not participate in protein biosynthesis although it is found in proteins in small amounts - particularly aged proteins and food proteins that have been processed. The biological functions of D-amino acids remain unclear, although D-phenylalanine has pharmacological activity at niacin receptor 2.[16]

DL-Phenylalanine (DLPA) is marketed as a nutritional supplement for its purported analgesic and antidepressant activities, which have been supported by clinical trials.[17][18][19] DL-Phenylalanine is a mixture of D-phenylalanine and L-phenylalanine. The reputed analgesic activity of DL-phenylalanine may be explained by the possible blockage by D-phenylalanine of enkephalin degradation by the enzyme carboxypeptidase A.[20][21] Enkephalins act as agonists of the mu and delta opioid receptors, and agonists of these receptors are known to produce antidepressant effects.[22] The mechanism of DL-phenylalanine's supposed antidepressant activity may also be accounted for in part by the precursor role of L-phenylalanine in the synthesis of the neurotransmitters norepinephrine and dopamine, though clinical trials have not found an antidepressant effect from L-phenylalanine alone.[17] Elevated brain levels of norepinephrine and dopamine are thought to have an antidepressant effect. D-Phenylalanine is absorbed from the small intestine and transported to the liver via the portal circulation. A small amount of D-phenylalanine appears to be converted to L-phenylalanine. D-Phenylalanine is distributed to the various tissues of the body via the systemic circulation. It appears to cross the blood–brain barrier less efficiently than L-phenylalanine, and so a small amount of an ingested dose of D-phenylalanine is excreted in the urine without penetrating the central nervous system.[23]

L-Phenylalanine is an antagonist at α2δ Ca2+ calcium channels with a Ki of 980 nM.[24]

In the brain, L-phenylalanine is a competitive antagonist at the glycine binding site of NMDA receptor[25] and at the glutamate binding site of AMPA receptor.[26] At the glycine binding site of NMDA receptor L-phenylalanine has an apparent equilibrium dissociation constant (KB) of 573 μM estimated by Schild regression[27] which is considerably lower than brain L-phenylalanine concentration observed in untreated human phenylketonuria.[28]L-Phenylalanine also inhibits neurotransmitter release at glutamatergic synapses in hippocampus and cortex with IC50 of 980 μM, a brain concentration seen in classical phenylketonuria, whereas D-phenylalanine has a significantly smaller effect.[26]

Commercial synthesis

L-Phenylalanine is produced for medical, feed, and nutritional applications, such as aspartame, in large quantities by utilizing the bacterium Escherichia coli, which naturally produces aromatic amino acids like phenylalanine. The quantity of L-phenylalanine produced commercially has been increased by genetically engineering E. coli, such as by altering the regulatory promoters or amplifying the number of genes controlling enzymes responsible for the synthesis of the amino acid.[29]

Derivatives

Boronophenylalanine (BPA) is a dihydroxyboryl derivative of phenylalanine, used in neutron capture therapy.

4-Azido-L-phenylalanine is a protein-incorporated unnatural amino acid used as a tool for bioconjugation in the field of chemical biology.

References

  1. ^ a b Ihlefeldt, Franziska Stefanie; Pettersen, Fredrik Bjarte; von Bonin, Aidan; Zawadzka, Malgorzata; Görbitz, Prof. Carl Henrik (2014). "The Polymorphs of L‐Phenylalanine". Angew. Chem. Int. Ed. 53 (49): 13600–13604. doi:10.1002/anie.201406886. PMID 25336255.
  2. ^ Dawson RM, et al. (1959). Data for Biochemical Research. Oxford: Clarendon Press.
  3. ^ . IUPAC-IUB Joint Commission on Biochemical Nomenclature. 1983. Archived from the original on 9 October 2008. Retrieved 5 March 2018.
  4. ^ Thorpe TE (1913). A Dictionary of Applied Chemistry. Longmans, Green, and Co. pp. 191–193. Retrieved 2012-06-04.
  5. ^ Plimmer RH (1912) [1908]. Plimmer RH, Hopkins FG (eds.). The Chemical Composition of the Proteins. Monographs on Biochemistry. Vol. Part I. Analysis (2nd ed.). London: Longmans, Green and Co. pp. 93–97. Retrieved 2012-06-04.
  6. ^ Ross HM, Roth J (1 April 1991). The Mood Control Diet: 21 Days to Conquering Depression and Fatigue. Simon & Schuster. p. 59. ISBN 978-0-13-590449-7.
  7. ^ Zeratsky, Katherine. "Phenylalanine in diet soda: Is it harmful?". Mayo Clinic. Retrieved 30 April 2019.
  8. ^ Institute of Medicine (2002). "Protein and Amino Acids". Dietary Reference Intakes for Energy, Carbohydrates, Fiber, Fat, Fatty Acids, Cholesterol, Protein, and Amino Acids. Washington, DC: The National Academies Press. pp. 589–768. doi:10.17226/10490. ISBN 978-0-309-08525-0.
  9. ^ Elango, Rajavel; Ball, Ronald O.; Pencharz, Paul B. (August 2012). "Recent advances in determining protein and amino acid requirements in humans". British Journal of Nutrition. 108 (S2): S22–S30. doi:10.1017/S0007114512002504. ISSN 0007-1145.
  10. ^ Eriksson, Johan G; Guzzardi, Maria-Angela; Iozzo, Patricia; Kajantie, Eero; Kautiainen, Hannu; Salonen, Minna K (2017-01-01). "Higher serum phenylalanine concentration is associated with more rapid telomere shortening in men". The American Journal of Clinical Nutrition. 105 (1): 144–150. doi:10.3945/ajcn.116.130468. ISSN 0002-9165. PMID 27881392.
  11. ^ Broadley KJ (March 2010). "The vascular effects of trace amines and amphetamines". Pharmacology & Therapeutics. 125 (3): 363–375. doi:10.1016/j.pharmthera.2009.11.005. PMID 19948186.
  12. ^ Lindemann L, Hoener MC (May 2005). "A renaissance in trace amines inspired by a novel GPCR family". Trends in Pharmacological Sciences. 26 (5): 274–281. doi:10.1016/j.tips.2005.03.007. PMID 15860375.
  13. ^ Wang X, Li J, Dong G, Yue J (February 2014). "The endogenous substrates of brain CYP2D". European Journal of Pharmacology. 724: 211–218. doi:10.1016/j.ejphar.2013.12.025. PMID 24374199.
  14. ^ Nelson DL, Cox MM (2000). Lehninger, Principles of Biochemistry (3rd ed.). New York: Worth Publishing. ISBN 1-57259-153-6.
  15. ^ . UK: Food Standards Agency. Archived from the original on 2012-02-21. Retrieved 2007-06-19.
  16. ^ "D-Phenylalanine: Biological activity". The IUPHAR/BPS Guide to PHARMACOLOGY. Retrieved 27 December 2018.
  17. ^ a b Wood, David R.; Reimherr, Fred W.; Wender, Paul H. (1985). "Treatment of attention deficit disorder with DL-phenylalanine". Psychiatry Research. Elsevier BV. 16 (1): 21–26. doi:10.1016/0165-1781(85)90024-1. ISSN 0165-1781. PMID 3903813. S2CID 3077060.
  18. ^ Beckmann, H.; Strauss, M. A.; Ludolph, E. (1977). "DL-Phenylalanine in depressed patients: An open study". Journal of Neural Transmission. Springer Science and Business Media LLC. 41 (2–3): 123–134. doi:10.1007/bf01670277. ISSN 0300-9564. PMID 335027. S2CID 5849451.
  19. ^ Beckmann, Helmut; Athen, Dieter; Olteanu, Margit; Zimmer, Reinhild (1979). "DL-Phenylalanine versus imipramine: A double-blind controlled study". Archiv für Psychiatrie und Nervenkrankheiten. Springer Science and Business Media LLC. 227 (1): 49–58. doi:10.1007/bf00585677. ISSN 0003-9373. PMID 387000. S2CID 23531579.
  20. ^ "D-Phenylalanine: Clinical data". The IUPHAR/BPS Guide to PHARMACOLOGY. Retrieved 27 December 2018.
  21. ^ Christianson DW, Mangani S, Shoham G, Lipscomb WN (August 1989). "Binding of D-phenylalanine and D-tyrosine to carboxypeptidase A" (PDF). The Journal of Biological Chemistry. 264 (22): 12849–12853. doi:10.1016/S0021-9258(18)51564-7. PMID 2568989.
  22. ^ Jelen, Luke A.; Stone, James M.; Young, Allan H.; Mehta, Mitul A. (2022). "The opioid system in depression". Neuroscience & Biobehavioral Reviews. Elsevier BV. 140: 104800. doi:10.1016/j.neubiorev.2022.104800. ISSN 0149-7634. PMID 35914624. S2CID 251163234.
  23. ^ Lehmann, W. D.; Theobald, N.; Fischer, R.; Heinrich, H. C. (1983-03-14). "Stereospecificity of phenylalanine plasma kinetics and hydroxylation in man following oral application of a stable isotope-labelled pseudo-racemic mixture of L- and D-phenylalanine". Clinica Chimica Acta; International Journal of Clinical Chemistry. 128 (2–3): 181–198. doi:10.1016/0009-8981(83)90319-4. ISSN 0009-8981. PMID 6851137.
  24. ^ Mortell KH, Anderson DJ, Lynch JJ, Nelson SL, Sarris K, McDonald H, Sabet R, Baker S, Honore P, Lee CH, Jarvis MF, Gopalakrishnan M (March 2006). "Structure-activity relationships of alpha-amino acid ligands for the alpha2delta subunit of voltage-gated calcium channels". Bioorganic & Medicinal Chemistry Letters. 16 (5): 1138–4111. doi:10.1016/j.bmcl.2005.11.108. PMID 16380257.
  25. ^ Glushakov AV, Dennis DM, Morey TE, Sumners C, Cucchiara RF, Seubert CN, Martynyuk AE (2002). "Specific inhibition of N-methyl-D-aspartate receptor function in rat hippocampal neurons by L-phenylalanine at concentrations observed during phenylketonuria". Molecular Psychiatry. 7 (4): 359–367. doi:10.1038/sj.mp.4000976. PMID 11986979.
  26. ^ a b Glushakov AV, Dennis DM, Sumners C, Seubert CN, Martynyuk AE (April 2003). "L-Phenylalanine selectively depresses currents at glutamatergic excitatory synapses". Journal of Neuroscience Research. 72 (1): 116–124. doi:10.1002/jnr.10569. PMID 12645085. S2CID 42087834.
  27. ^ Glushakov AV, Glushakova O, Varshney M, Bajpai LK, Sumners C, Laipis PJ, Embury JE, Baker SP, Otero DH, Dennis DM, Seubert CN, Martynyuk AE (February 2005). "Long-term changes in glutamatergic synaptic transmission in phenylketonuria". Brain. 128 (Pt 2): 300–307. doi:10.1093/brain/awh354. PMID 15634735.
  28. ^ Möller HE, Weglage J, Bick U, Wiedermann D, Feldmann R, Ullrich K (December 2003). "Brain imaging and proton magnetic resonance spectroscopy in patients with phenylketonuria". Pediatrics. 112 (6 Pt 2): 1580–1583. doi:10.1542/peds.112.S4.1580. hdl:11858/00-001M-0000-0010-A24A-C. PMID 14654669. S2CID 2198040.
  29. ^ Sprenger GA (2007). "Aromatic Amino Acids". Amino Acid Biosynthesis: Pathways, Regulation and Metabolic Engineering (1st ed.). Springer. pp. 106–113. ISBN 978-3-540-48595-7.

External links

 
Wikimedia Commons has media related to L-Phenylalanine.
  • Phenylalanine mass spectrum
  • Phenylalanine at ChemSynthesis

May 19, 2023
phenylalanine, symbol, essential, amino, acid, with, formula, viewed, benzyl, group, substituted, methyl, group, alanine, phenyl, group, place, terminal, hydrogen, alanine, this, essential, amino, acid, classified, neutral, nonpolar, because, inert, hydrophobi. Phenylalanine symbol Phe or F 3 is an essential a amino acid with the formula C9 H11 NO2 It can be viewed as a benzyl group substituted for the methyl group of alanine or a phenyl group in place of a terminal hydrogen of alanine This essential amino acid is classified as neutral and nonpolar because of the inert and hydrophobic nature of the benzyl side chain The L isomer is used to biochemically form proteins coded for by DNA Phenylalanine is a precursor for tyrosine the monoamine neurotransmitters dopamine norepinephrine noradrenaline and epinephrine adrenaline and the skin pigment melanin It is encoded by the codons UUU and UUC Phenylalanine Skeletal formula of L phenylalanineL Phenylalanine at physiological pHBall and stick model 1 Space filling model 1 NamesPronunciation US ˌ f ɛ n el ˈ ae l e n iː n UK ˌ f iː n aɪ l IUPAC name PhenylalanineSystematic IUPAC name S 2 Amino 3 phenylpropanoic acidIdentifiersCAS Number L 63 91 2 YD L 150 30 1 YD 673 06 3 Y3D model JSmol L Interactive imageL Zwitterion Interactive imageChEBI L CHEBI 17295 YD CHEBI 16998 YChEMBL L ChEMBL301523 YChemSpider L 5910 YD L 969 YD 64639 YDrugBank L DB00120 YECHA InfoCard 100 000 517IUPHAR BPS L 3313KEGG L D00021 YPubChem CID L 6140D L 994D 71567UNII L 47E5O17Y3R YD L 8P946UF12S YD 032K16VRCU YCompTox Dashboard EPA L DTXSID4040763InChI InChI 1S C9H11NO2 c10 8 9 11 12 6 7 4 2 1 3 5 7 h1 5 8H 6 10H2 H 11 12 t8 m0 s1 YKey COLNVLDHVKWLRT QMMMGPOBSA N YL Key COLNVLDHVKWLRT QMMMGPOBBCD L Key COLNVLDHVKWLRT UHFFFAOYSA ND Key COLNVLDHVKWLRT MRVPVSSYSA NSMILES L c1ccc cc1 C C H C O O NL Zwitterion NH3 C H CC1 CC CC C1 C O OPropertiesChemical formula C 9H 11N O 2Molar mass 165 192 g mol 1Acidity pKa 1 83 carboxyl 9 13 amino 2 HazardsNFPA 704 fire diamond 210Supplementary data pagePhenylalanine data page Except where otherwise noted data are given for materials in their standard state at 25 C 77 F 100 kPa Infobox references Phenylalanine is found naturally in the milk of mammals It is used in the manufacture of food and drink products and sold as a nutritional supplement for its analgesic and antidepressant effects It is a direct precursor to the neuromodulator phenethylamine a commonly used dietary supplement As an essential amino acid phenylalanine is not synthesized de novo in humans and other animals who must ingest phenylalanine or phenylalanine containing proteins Contents 1 History 2 Dietary sources 3 Dietary recommendations 4 Other biological roles 4 1 In plants 5 Biosynthesis 6 Phenylketonuria 7 D L and DL phenylalanine 8 Commercial synthesis 9 Derivatives 10 References 11 External linksHistory EditThe first description of phenylalanine was made in 1879 when Schulze and Barbieri identified a compound with the empirical formula C9H11NO2 in yellow lupine Lupinus luteus seedlings In 1882 Erlenmeyer and Lipp first synthesized phenylalanine from phenylacetaldehyde hydrogen cyanide and ammonia 4 5 The genetic codon for phenylalanine was first discovered by J Heinrich Matthaei and Marshall W Nirenberg in 1961 They showed that by using mRNA to insert multiple uracil repeats into the genome of the bacterium E coli they could cause the bacterium to produce a polypeptide consisting solely of repeated phenylalanine amino acids This discovery helped to establish the nature of the coding relationship that links information stored in genomic nucleic acid with protein expression in the living cell Dietary sources EditGood sources of phenylalanine are eggs chicken liver beef milk and soybeans 6 Another common source of phenylalanine is anything sweetened with the artificial sweetener aspartame such as diet drinks diet foods and medication the metabolism of aspartame produces phenylalanine as one of the compound s metabolites 7 Dietary recommendations EditThe Food and Nutrition Board FNB of the U S Institute of Medicine set Recommended Dietary Allowances RDAs for essential amino acids in 2002 For phenylalanine plus tyrosine for adults 19 years and older 33 mg kg body weight day 8 In 2005 the DRI is set to 27 mg kg per day with no tyrosine the FAO WHO UNU recommendation of 2007 is 25 mg kg per day with no tyrosine 9 Other biological roles EditL Phenylalanine is biologically converted into L tyrosine another one of the DNA encoded amino acids L tyrosine in turn is converted into L DOPA which is further converted into dopamine norepinephrine noradrenaline and epinephrine adrenaline The latter three are known as the catecholamines Phenylalanine uses the same active transport channel as tryptophan to cross the blood brain barrier In excessive quantities supplementation can interfere with the production of serotonin and other aromatic amino acids 10 as well as nitric oxide due to the overuse eventually limited availability of the associated cofactors iron or tetrahydrobiopterin citation needed The corresponding enzymes for those compounds are the aromatic amino acid hydroxylase family and nitric oxide synthase Biosynthetic pathways for catecholamines and trace amines in the human brain 11 12 13 L Phenylalanine L Tyrosine L DOPA Epinephrine Phenethylamine p Tyramine Dopamine Norepinephrine N Methylphenethylamine N Methyltyramine p Octopamine Synephrine 3 Methoxytyramine AADC AADC AADC primarypathway PNMT PNMT PNMT PNMT AAAH AAAH brainCYP2D6 minorpathway COMT DBH DBH Phenylalanine in humans may ultimately be metabolized into a range of different substances In plants Edit Phenylalanine is the starting compound used in the synthesis of flavonoids Lignan is derived from phenylalanine and from tyrosine Phenylalanine is converted to cinnamic acid by the enzyme phenylalanine ammonia lyase 14 Biosynthesis EditPhenylalanine is biosynthesized via the Shikimate pathway Phenylketonuria EditMain article Phenylketonuria The genetic disorder phenylketonuria PKU is the inability to metabolize phenylalanine because of a lack of the enzyme phenylalanine hydroxylase Individuals with this disorder are known as phenylketonurics and must regulate their intake of phenylalanine Phenylketonurics often use blood tests to monitor the amount of phenylalanine in their blood Lab results may report phenylalanine levels using either mg dL and mmol L One mg dL of phenylalanine is approximately equivalent to 60 mmol L A rare variant form of phenylketonuria called hyperphenylalaninemia is caused by the inability to synthesize a cofactor called tetrahydrobiopterin which can be supplemented Pregnant women with hyperphenylalaninemia may show similar symptoms of the disorder high levels of phenylalanine in blood but these indicators will usually disappear at the end of gestation Pregnant women with PKU must control their blood phenylalanine levels even if the fetus is heterozygous for the defective gene because the fetus could be adversely affected due to hepatic immaturity medical citation needed A non food source of phenylalanine is the artificial sweetener aspartame This compound is metabolized by the body into several chemical byproducts including phenylalanine The breakdown problems phenylketonurics have with the buildup of phenylalanine in the body also occurs with the ingestion of aspartame although to a lesser degree Accordingly all products in Australia the U S and Canada that contain aspartame must be labeled Phenylketonurics Contains phenylalanine In the UK foods containing aspartame must carry ingredient panels that refer to the presence of aspartame or E951 15 and they must be labeled with a warning Contains a source of phenylalanine In Brazil the label Contem Fenilalanina Portuguese for Contains Phenylalanine is also mandatory in products which contain it These warnings are placed to help individuals avoid such foods D L and DL phenylalanine EditThe stereoisomer D phenylalanine DPA can be produced by conventional organic synthesis either as a single enantiomer or as a component of the racemic mixture It does not participate in protein biosynthesis although it is found in proteins in small amounts particularly aged proteins and food proteins that have been processed The biological functions of D amino acids remain unclear although D phenylalanine has pharmacological activity at niacin receptor 2 16 DL Phenylalanine DLPA is marketed as a nutritional supplement for its purported analgesic and antidepressant activities which have been supported by clinical trials 17 18 19 DL Phenylalanine is a mixture of D phenylalanine and L phenylalanine The reputed analgesic activity of DL phenylalanine may be explained by the possible blockage by D phenylalanine of enkephalin degradation by the enzyme carboxypeptidase A 20 21 Enkephalins act as agonists of the mu and delta opioid receptors and agonists of these receptors are known to produce antidepressant effects 22 The mechanism of DL phenylalanine s supposed antidepressant activity may also be accounted for in part by the precursor role of L phenylalanine in the synthesis of the neurotransmitters norepinephrine and dopamine though clinical trials have not found an antidepressant effect from L phenylalanine alone 17 Elevated brain levels of norepinephrine and dopamine are thought to have an antidepressant effect D Phenylalanine is absorbed from the small intestine and transported to the liver via the portal circulation A small amount of D phenylalanine appears to be converted to L phenylalanine D Phenylalanine is distributed to the various tissues of the body via the systemic circulation It appears to cross the blood brain barrier less efficiently than L phenylalanine and so a small amount of an ingested dose of D phenylalanine is excreted in the urine without penetrating the central nervous system 23 L Phenylalanine is an antagonist at a2d Ca2 calcium channels with a Ki of 980 nM 24 In the brain L phenylalanine is a competitive antagonist at the glycine binding site of NMDA receptor 25 and at the glutamate binding site of AMPA receptor 26 At the glycine binding site of NMDA receptor L phenylalanine has an apparent equilibrium dissociation constant KB of 573 mM estimated by Schild regression 27 which is considerably lower than brain L phenylalanine concentration observed in untreated human phenylketonuria 28 L Phenylalanine also inhibits neurotransmitter release at glutamatergic synapses in hippocampus and cortex with IC50 of 980 mM a brain concentration seen in classical phenylketonuria whereas D phenylalanine has a significantly smaller effect 26 Commercial synthesis EditL Phenylalanine is produced for medical feed and nutritional applications such as aspartame in large quantities by utilizing the bacterium Escherichia coli which naturally produces aromatic amino acids like phenylalanine The quantity of L phenylalanine produced commercially has been increased by genetically engineering E coli such as by altering the regulatory promoters or amplifying the number of genes controlling enzymes responsible for the synthesis of the amino acid 29 Derivatives EditBoronophenylalanine BPA is a dihydroxyboryl derivative of phenylalanine used in neutron capture therapy 4 Azido L phenylalanine is a protein incorporated unnatural amino acid used as a tool for bioconjugation in the field of chemical biology References Edit a b Ihlefeldt Franziska Stefanie Pettersen Fredrik Bjarte von Bonin Aidan Zawadzka Malgorzata Gorbitz Prof Carl Henrik 2014 The Polymorphs of L Phenylalanine Angew Chem Int Ed 53 49 13600 13604 doi 10 1002 anie 201406886 PMID 25336255 Dawson RM et al 1959 Data for Biochemical Research Oxford Clarendon Press Nomenclature and Symbolism for Amino Acids and Peptides IUPAC IUB Joint Commission on Biochemical Nomenclature 1983 Archived from the original on 9 October 2008 Retrieved 5 March 2018 Thorpe TE 1913 A Dictionary of Applied Chemistry Longmans Green and Co pp 191 193 Retrieved 2012 06 04 Plimmer RH 1912 1908 Plimmer RH Hopkins FG eds The Chemical Composition of the Proteins Monographs on Biochemistry Vol Part I Analysis 2nd ed London Longmans Green and Co pp 93 97 Retrieved 2012 06 04 Ross HM Roth J 1 April 1991 The Mood Control Diet 21 Days to Conquering Depression and Fatigue Simon amp Schuster p 59 ISBN 978 0 13 590449 7 Zeratsky Katherine Phenylalanine in diet soda Is it harmful Mayo Clinic Retrieved 30 April 2019 Institute of Medicine 2002 Protein and Amino Acids Dietary Reference Intakes for Energy Carbohydrates Fiber Fat Fatty Acids Cholesterol Protein and Amino Acids Washington DC The National Academies Press pp 589 768 doi 10 17226 10490 ISBN 978 0 309 08525 0 Elango Rajavel Ball Ronald O Pencharz Paul B August 2012 Recent advances in determining protein and amino acid requirements in humans British Journal of Nutrition 108 S2 S22 S30 doi 10 1017 S0007114512002504 ISSN 0007 1145 Eriksson Johan G Guzzardi Maria Angela Iozzo Patricia Kajantie Eero Kautiainen Hannu Salonen Minna K 2017 01 01 Higher serum phenylalanine concentration is associated with more rapid telomere shortening in men The American Journal of Clinical Nutrition 105 1 144 150 doi 10 3945 ajcn 116 130468 ISSN 0002 9165 PMID 27881392 Broadley KJ March 2010 The vascular effects of trace amines and amphetamines Pharmacology amp Therapeutics 125 3 363 375 doi 10 1016 j pharmthera 2009 11 005 PMID 19948186 Lindemann L Hoener MC May 2005 A renaissance in trace amines inspired by a novel GPCR family Trends in Pharmacological Sciences 26 5 274 281 doi 10 1016 j tips 2005 03 007 PMID 15860375 Wang X Li J Dong G Yue J February 2014 The endogenous substrates of brain CYP2D European Journal of Pharmacology 724 211 218 doi 10 1016 j ejphar 2013 12 025 PMID 24374199 Nelson DL Cox MM 2000 Lehninger Principles of Biochemistry 3rd ed New York Worth Publishing ISBN 1 57259 153 6 Aspartame UK Food Standards Agency Archived from the original on 2012 02 21 Retrieved 2007 06 19 D Phenylalanine Biological activity The IUPHAR BPS Guide to PHARMACOLOGY Retrieved 27 December 2018 a b Wood David R Reimherr Fred W Wender Paul H 1985 Treatment of attention deficit disorder with DL phenylalanine Psychiatry Research Elsevier BV 16 1 21 26 doi 10 1016 0165 1781 85 90024 1 ISSN 0165 1781 PMID 3903813 S2CID 3077060 Beckmann H Strauss M A Ludolph E 1977 DL Phenylalanine in depressed patients An open study Journal of Neural Transmission Springer Science and Business Media LLC 41 2 3 123 134 doi 10 1007 bf01670277 ISSN 0300 9564 PMID 335027 S2CID 5849451 Beckmann Helmut Athen Dieter Olteanu Margit Zimmer Reinhild 1979 DL Phenylalanine versus imipramine A double blind controlled study Archiv fur Psychiatrie und Nervenkrankheiten Springer Science and Business Media LLC 227 1 49 58 doi 10 1007 bf00585677 ISSN 0003 9373 PMID 387000 S2CID 23531579 D Phenylalanine Clinical data The IUPHAR BPS Guide to PHARMACOLOGY Retrieved 27 December 2018 Christianson DW Mangani S Shoham G Lipscomb WN August 1989 Binding of D phenylalanine and D tyrosine to carboxypeptidase A PDF The Journal of Biological Chemistry 264 22 12849 12853 doi 10 1016 S0021 9258 18 51564 7 PMID 2568989 Jelen Luke A Stone James M Young Allan H Mehta Mitul A 2022 The opioid system in depression Neuroscience amp Biobehavioral Reviews Elsevier BV 140 104800 doi 10 1016 j neubiorev 2022 104800 ISSN 0149 7634 PMID 35914624 S2CID 251163234 Lehmann W D Theobald N Fischer R Heinrich H C 1983 03 14 Stereospecificity of phenylalanine plasma kinetics and hydroxylation in man following oral application of a stable isotope labelled pseudo racemic mixture of L and D phenylalanine Clinica Chimica Acta International Journal of Clinical Chemistry 128 2 3 181 198 doi 10 1016 0009 8981 83 90319 4 ISSN 0009 8981 PMID 6851137 Mortell KH Anderson DJ Lynch JJ Nelson SL Sarris K McDonald H Sabet R Baker S Honore P Lee CH Jarvis MF Gopalakrishnan M March 2006 Structure activity relationships of alpha amino acid ligands for the alpha2delta subunit of voltage gated calcium channels Bioorganic amp Medicinal Chemistry Letters 16 5 1138 4111 doi 10 1016 j bmcl 2005 11 108 PMID 16380257 Glushakov AV Dennis DM Morey TE Sumners C Cucchiara RF Seubert CN Martynyuk AE 2002 Specific inhibition of N methyl D aspartate receptor function in rat hippocampal neurons by L phenylalanine at concentrations observed during phenylketonuria Molecular Psychiatry 7 4 359 367 doi 10 1038 sj mp 4000976 PMID 11986979 a b Glushakov AV Dennis DM Sumners C Seubert CN Martynyuk AE April 2003 L Phenylalanine selectively depresses currents at glutamatergic excitatory synapses Journal of Neuroscience Research 72 1 116 124 doi 10 1002 jnr 10569 PMID 12645085 S2CID 42087834 Glushakov AV Glushakova O Varshney M Bajpai LK Sumners C Laipis PJ Embury JE Baker SP Otero DH Dennis DM Seubert CN Martynyuk AE February 2005 Long term changes in glutamatergic synaptic transmission in phenylketonuria Brain 128 Pt 2 300 307 doi 10 1093 brain awh354 PMID 15634735 Moller HE Weglage J Bick U Wiedermann D Feldmann R Ullrich K December 2003 Brain imaging and proton magnetic resonance spectroscopy in patients with phenylketonuria Pediatrics 112 6 Pt 2 1580 1583 doi 10 1542 peds 112 S4 1580 hdl 11858 00 001M 0000 0010 A24A C PMID 14654669 S2CID 2198040 Sprenger GA 2007 Aromatic Amino Acids Amino Acid Biosynthesis Pathways Regulation and Metabolic Engineering 1st ed Springer pp 106 113 ISBN 978 3 540 48595 7 External links Edit Wikimedia Commons has media related to L Phenylalanine Phenylalanine mass spectrum Phenylalanine at ChemSynthesis Retrieved from https en wikipedia org w index php title Phenylalanine amp oldid 1151217460, wikipedia, wiki, book, books, library,

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