Chemistry:Methionine

From HandWiki
Short description: Sulfur-containing amino acid
Methionine
Chemical structure of methionine
Skeletal formula of the canonical form of methionine
Methionine-from-xtal-3D-bs-17.png
L-methionine-from-xtal-Mercury-3D-sf.png
Names
IUPAC name
Methionine
Other names
2-amino-4-(methylthio)butanoic acid
Identifiers
3D model (JSmol)
Abbreviations Met, M
ChEBI
ChEMBL
ChemSpider
DrugBank
EC Number
  • L: 200-432-1
KEGG
UNII
Properties[2]
C5H11NO2S
Molar mass 149.21 g·mol−1
Appearance White crystalline powder
Density 1.340 g/cm3
Melting point 281 °C (538 °F; 554 K) decomposes
Soluble
Acidity (pKa) 2.28 (carboxyl), 9.21 (amino)[1]
Pharmacology
1=ATC code }} V03AB26 (WHO) QA05BA90 (WHO), QG04BA90 (WHO)
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa).
Infobox references
Tracking categories (test):

Methionine (symbol Met or M)[3] (/mɪˈθənn/)[4] is an essential amino acid in humans.

As the precursor of other non-essential amino acids such as cysteine and taurine, versatile compounds such as SAM-e, and the important antioxidant glutathione, methionine plays a critical role in the metabolism and health of many species, including humans. Methionine is also involved in angiogenesis and various processes related to DNA transcription, epigenetic expression, and gene regulation.

Methionine was first isolated in 1921 by John Howard Mueller.[5] It is encoded by the codon AUG.

Biochemical details

Methionine (abbreviated as Met or M; encoded by the codon AUG) is an α-amino acid that is used in the biosynthesis of proteins. It contains a carboxyl group (which is in the deprotonated −COO form under biological pH conditions), an amino group (which is in the protonated −NH+3 form under biological pH conditions) located in α-position with respect to the carboxyl group, and an S-methyl thioether side chain, classifying it as a nonpolar, aliphatic amino acid.

In nuclear genes of eukaryotes and in Archaea, methionine is coded for by the start codon, meaning it indicates the start of the coding region and is the first amino acid produced in a nascent polypeptide during mRNA translation.[6]

A proteinogenic amino acid

Cysteine and methionine are the two sulfur-containing proteinogenic amino acids. Excluding the few exceptions where methionine may act as a redox sensor (e.g.,methionine sulfoxide[7]), methionine residues do not have a catalytic role.[8] This is in contrast to cysteine residues, where the thiol group has a catalytic role in many proteins.[8] The thioether within methionine does however have a minor structural role due to the stability effect of S/π interactions between the side chain sulfur atom and aromatic amino acids in one-third of all known protein structures.[8] This lack of a strong role is reflected in experiments where little effect is seen in proteins where methionine is replaced by norleucine, a straight hydrocarbon sidechain amino acid which lacks the thioether.[9] It has been conjectured that norleucine was present in early versions of the genetic code, but methionine intruded into the final version of the genetic code due to the fact it is used in the cofactor S-adenosylmethionine (SAM-e).[10] This situation is not unique and may have occurred with ornithine and arginine.[11]

Encoding

Methionine is one of only two amino acids encoded by a single codon (AUG) in the standard genetic code (tryptophan, encoded by UGG, is the other). In reflection to the evolutionary origin of its codon, the other AUN codons encode isoleucine, which is also a hydrophobic amino acid. In the mitochondrial genome of several organisms, including metazoa and yeast, the codon AUA also encodes for methionine. In the standard genetic code AUA codes for isoleucine and the respective tRNA (ileX in Escherichia coli) uses the unusual base lysidine (bacteria) or agmatidine (archaea) to discriminate against AUG.[12][13]

The methionine codon AUG is also the most common start codon. A "Start" codon is message for a ribosome that signals the initiation of protein translation from mRNA when the AUG codon is in a Kozak consensus sequence. As a consequence, methionine is often incorporated into the N-terminal position of proteins in eukaryotes and archaea during translation, although it can be removed by post-translational modification. In bacteria, the derivative N-formylmethionine is used as the initial amino acid.

Derivatives

S-Adenosylmethionine

S-Adenosylmethionine is a cofactor derived from methionine.

The methionine-derivative S-adenosylmethionine (SAM-e) is a cofactor that serves mainly as a methyl donor. SAM-e is composed of an adenosyl molecule (via 5′ carbon) attached to the sulfur of methionine, therefore making it a sulfonium cation (i.e., three substituents and positive charge). The sulfur acts as a soft Lewis acid (i.e., donor/electrophile) which allows the S-methyl group to be transferred to an oxygen, nitrogen, or aromatic system, often with the aid of other cofactors such as cobalamin (vitamin B12 in humans). Some enzymes use SAM-e to initiate a radical reaction; these are called radical SAM-e enzymes. As a result of the transfer of the methyl group, S-adenosylhomocysteine is obtained. In bacteria, this is either regenerated by methylation or is salvaged by removing the adenine and the homocysteine, leaving the compound dihydroxypentandione to spontaneously convert into autoinducer-2, which is excreted as a waste product or quorum signal.

Biosynthesis

Methionine biosynthesis

As an essential amino acid, methionine is not synthesized de novo in humans and other animals, which must ingest methionine or methionine-containing proteins. In plants and microorganisms, methionine biosynthesis belongs to the aspartate family, along with threonine and lysine (via diaminopimelate, but not via α-aminoadipate). The main backbone is derived from aspartic acid, while the sulfur may come from cysteine, methanethiol, or hydrogen sulfide.[8]

  • First, aspartic acid is converted via β-aspartyl semialdehyde into homoserine by two reduction steps of the terminal carboxyl group (homoserine has therefore a γ-hydroxyl, hence the homo- series). The intermediate aspartate semialdehyde is the branching point with the lysine biosynthetic pathway, where it is instead condensed with pyruvate. Homoserine is the branching point with the threonine pathway, where instead it is isomerised after activating the terminal hydroxyl with phosphate (also used for methionine biosynthesis in plants).[8]
  • Homoserine is then activated with a phosphate, succinyl or an acetyl group on the hydroxyl.
    • In plants and possibly in some bacteria,[8] phosphate is used. This step is shared with threonine biosynthesis.[8]
    • In most organisms, an acetyl group is used to activate the homoserine. This can be catalysed in bacteria by an enzyme encoded by metX or metA (not homologues).[8]
    • In enterobacteria and a limited number of other organisms, succinate is used. The enzyme that catalyses the reaction is MetA and the specificity for acetyl-CoA and succinyl-CoA is dictated by a single residue.[8] The physiological basis for the preference of acetyl-CoA or succinyl-CoA is unknown, but such alternative routes are present in some other pathways (e.g. lysine biosynthesis and arginine biosynthesis).
  • The hydroxyl activating group is then replaced with cysteine, methanethiol, or hydrogen sulfide. A replacement reaction is technically a γ-elimination followed by a variant of a Michael addition. All the enzymes involved are homologues and members of the Cys/Met metabolism PLP-dependent enzyme family, which is a subset of the PLP-dependent fold type I clade. They utilise the cofactor PLP (pyridoxal phosphate), which functions by stabilising carbanion intermediates.[8]
    • If it reacts with cysteine, it produces cystathionine, which is cleaved to yield homocysteine. The enzymes involved are cystathionine-γ-synthase (encoded by metB in bacteria) and cystathionine-β-lyase (metC). Cystathionine is bound differently in the two enzymes allowing β or γ reactions to occur.[8]
    • If it reacts with free hydrogen sulfide, it produces homocysteine. This is catalysed by O-acetylhomoserine aminocarboxypropyltransferase (formerly known as O-acetylhomoserine (thiol)-lyase. It is encoded by either metY or metZ in bacteria.[8]
    • If it reacts with methanethiol, it produces methionine directly. Methanethiol is a byproduct of catabolic pathway of certain compounds, therefore this route is more uncommon.[8]
  • If homocysteine is produced, the thiol group is methylated, yielding methionine. Two methionine synthases are known; one is cobalamin (vitamin B12) dependent and one is independent.[8]

The pathway using cysteine is called the "transsulfuration pathway", while the pathway using hydrogen sulfide (or methanethiol) is called "direct-sulfurylation pathway".

Cysteine is similarly produced, namely it can be made from an activated serine and either from homocysteine ("reverse transsulfurylation route") or from hydrogen sulfide ("direct sulfurylation route"); the activated serine is generally O-acetylserine (via CysK or CysM in E. coli), but in Aeropyrum pernix and some other archaea O-phosphoserine is used.[14] CysK and CysM are homologues, but belong to the PLP fold type III clade.

Transsulfurylation pathway

Main page: Biology:Transsulfuration pathway

Enzymes involved in the E. coli transsulfurylation route of methionine biosynthesis:

  1. Aspartokinase
  2. Aspartate-semialdehyde dehydrogenase
  3. Homoserine dehydrogenase
  4. Homoserine O-transsuccinylase
  5. Cystathionine-γ-synthase
  6. Cystathionine-β-lyase
  7. Methionine synthase (in mammals, this step is performed by homocysteine methyltransferase or betaine—homocysteine S-methyltransferase.)

Other biochemical pathways

Fates of methionine

Although mammals cannot synthesize methionine, they can still use it in a variety of biochemical pathways:

Catabolism

Methionine is converted to S-adenosylmethionine (SAM-e) by (1) methionine adenosyltransferase.

SAM-e serves as a methyl donor in many (2) methyltransferase reactions, and is converted to S-adenosylhomocysteine (SAH).

(3) Adenosylhomocysteinase cysteine.

Regeneration

Methionine can be regenerated from homocysteine via (4) methionine synthase in a reaction that requires vitamin B12 as a cofactor.

Homocysteine can also be remethylated using glycine betaine (N,N,N-trimethylglycine, TMG) to methionine via the enzyme betaine-homocysteine methyltransferase (E.C.2.1.1.5, BHMT). BHMT makes up to 1.5% of all the soluble protein of the liver, and recent evidence suggests that it may have a greater influence on methionine and homocysteine homeostasis than methionine synthase.

Reverse-transulfurylation pathway: conversion to cysteine

Homocysteine can be converted to cysteine.

  • (5) Cystathionine-β-synthase (an enzyme which requires pyridoxal phosphate, the active form of vitamin B6) combines homocysteine and serine to produce cystathionine. Instead of degrading cystathionine via cystathionine-β-lyase, as in the biosynthetic pathway, cystathionine is broken down to cysteine and α-ketobutyrate via (6) cystathionine-γ-lyase.
  • (7) The enzyme α-ketoacid dehydrogenase converts α-ketobutyrate to propionyl-CoA, which is metabolized to succinyl-CoA in a three-step process (see propionyl-CoA for pathway).

Ethylene synthesis

This amino acid is also used by plants for synthesis of ethylene. The process is known as the Yang cycle or the methionine cycle.

The Yang cycle

Metabolic diseases

The degradation of methionine is impaired in the following metabolic diseases:

Chemical synthesis

The industrial synthesis combines acrolein, methanethiol, and cyanide, which affords the hydantoin.[15] Racemic methionine can also be synthesized from diethyl sodium phthalimidomalonate by alkylation with chloroethylmethylsulfide (ClCH2CH2SCH3) followed by hydrolysis and decarboxylation. Also see Methanol. [16]

Human nutrition

Methionine supplementation benefit those suffering from copper poisoning.[17]

Overconsumption of methionine, the methyl group donor in DNA methylation, is related to cancer growth in a number of studies.[18][19]

Requirements

The Food and Nutrition Board of the U.S. Institute of Medicine set Recommended Dietary Allowances (RDAs) for essential amino acids in 2002. For methionine combined with cysteine, for adults 19 years and older, 19 mg/kg body weight/day.[20]

This translates to about 1.33 grams per day for a 70 kilogram individual.

Dietary sources

Food sources of methionine[citation needed]
Food g/100 g
Egg, white, dried, powder, glucose reduced 3.204
Sesame seeds flour (low fat) 1.656
Brazil nuts 1.124
Cheese, Parmesan, shredded 1.114
hemp seed, hulled 0.933
Soy protein concentrate 0.814
Chicken, broilers or fryers, roasted 0.801
Fish, tuna, light, canned in water, drained solids 0.755
Beef, cured, dried 0.749
Bacon 0.593
chia seeds 0.588
Beef, ground, 95% lean meat / 5% fat, raw 0.565
Pork, ground, 96% lean / 4% fat, raw 0.564
Soybeans 0.547
Wheat germ 0.456
Egg, whole, cooked, hard-boiled 0.392
Oat 0.312
Peanuts 0.309
Chickpea 0.253
Corn, yellow 0.197
Almonds 0.151
Beans, pinto, cooked 0.117
Lentils, cooked 0.077
Rice, brown, medium-grain, cooked 0.052

High levels of methionine can be found in eggs, meat, and fish; sesame seeds, Brazil nuts, and some other plant seeds; and cereal grains. Most fruits and vegetables contain very little. Most legumes, though protein dense, are low in methionine. Proteins without adequate methionine are not considered to be complete proteins.[21] For that reason, racemic methionine is sometimes added as an ingredient to pet foods.[22]

Restriction

Some scientific evidence indicates restricting methionine consumption can increase lifespans in fruit flies.[23]

A 2005 study showed methionine restriction without energy restriction extends mouse lifespans.[24] This extension requires intact growth hormone signaling, as animals without intact growth-hormone signaling do not have a further increase in lifespan when methionine restricted.[25] The metabolic response to methionine restriction is also altered in mouse growth hormone signaling mutants.[26]

A study published in Nature showed adding just the essential amino acid methionine to the diet of fruit flies under dietary restriction, including restriction of essential amino acids (EAAs), restored fertility without reducing the longer lifespans that are typical of dietary restriction, leading the researchers to determine that methionine "acts in combination with one or more other EAAs to shorten lifespan."[23][27][28] Restoring methionine to the diet of mice on a dietary restriction regimen blocks many acute benefits of dietary restriction, a process that may be mediated by increased production of hydrogen sulfide.[29]

Methionine restriction can increase circulating liver hormone FGF21 between 5-fold and 10-fold in mice.[30] Several studies showed that methionine restriction also inhibits aging-related disease processes in mice[31][32] and inhibits colon carcinogenesis in rats.[33] In humans, methionine restriction through dietary modification could be achieved through a plant-based diet.[34]

Restriction of dietary methionine reduces levels of its catabolite S-adenosylmethionine (SAM-e), resulting is a subsequent loss of histone methylation.[35] An active process mediated by a specific, preserved methylation of H3K9 preserves the memory of the original methylation profile, allowing the epigenome to be restored when dietary methionine levels return.[35]

A 2009 study on rats showed "methionine supplementation in the diet specifically increases mitochondrial ROS production and mitochondrial DNA oxidative damage in rat liver mitochondria offering a plausible mechanism for its hepatotoxicity".[36]

Rats fed a diet without methionine and choline developed steatohepatitis (fatty liver) and anemia, and lost two-thirds of their body weight over 5 weeks. Administration of methionine ameliorated the pathological consequences of methionine deprivation.[37] Short-term removal of only methionine from the diet can reverse diet-induced obesity and promotes insulin sensitivity in mice,[38] and methionine restriction also protects a mouse model of spontaneous, polygenic obesity and diabetes.[39]

Health

Loss of methionine has been linked to senile greying of hair. Its lack leads to a buildup of hydrogen peroxide in hair follicles, a reduction in tyrosinase effectiveness, and a gradual loss of hair color.[40] Methionine raises the intracellular concentration of glutathione, thereby promoting antioxidant-mediated cell defense and redox regulation. It also protects cells against dopamine induced nigral cell loss by binding oxidative metabolites.[41]

Methionine is an intermediate in the biosynthesis of cysteine, carnitine, taurine, lecithin, phosphatidylcholine, and other phospholipids. Improper conversion of methionine can lead to atherosclerosis[42] due to accumulation of homocysteine.

Other uses

DL-Methionine is sometimes given as a supplement to dogs; It helps reduce the chances of kidney stones in dogs. Methionine is also known to increase the urinary excretion of quinidine by acidifying the urine. Aminoglycoside antibiotics used to treat urinary tract infections work best in alkaline conditions, and urinary acidification from using methionine can reduce its effectiveness. If a dog is on a diet that acidifies the urine, methionine should not be used.[43]

Methionine is allowed as a supplement to organic poultry feed under the US certified organic program.[44]

Methionine can be used as a nontoxic pesticide option against giant swallowtail caterpillars, which are a serious pest to orange crops.[45]

See also

References

  1. Dawson, Rex M. C.; Elliott, Daphne C.; Elliott, William H.; Jones, K. M. (1959). Data for Biochemical Research. Oxford: Clarendon Press. 
  2. Weast, Robert C., ed (1981). CRC Handbook of Chemistry and Physics (62nd ed.). Boca Raton, FL: CRC Press. p. C-374. ISBN 0-8493-0462-8. .
  3. "Nomenclature and Symbolism for Amino Acids and Peptides". IUPAC-IUB Joint Commission on Biochemical Nomenclature. 1983. http://www.chem.qmul.ac.uk/iupac/AminoAcid/AA1n2.html. 
  4. "Methionine". Oxford University Press. https://en.oxforddictionaries.com/definition/methionine. 
  5. "A Biographical Memoir of John Howard Mueller". Washington D.C.: National Academy of Sciences. 1987. http://www.nasonline.org/publications/biographical-memoirs/memoir-pdfs/mueller-john.pdf. 
  6. "Amino acids biosynthesis and nitrogen assimilation pathways: a great genomic deletion during eukaryotes evolution". BMC Genomics 12 (Suppl 4): S2. December 2011. doi:10.1186/1471-2164-12-S4-S2. PMID 22369087. 
  7. "Redox modulation of cellular signaling and metabolism through reversible oxidation of methionine sensors in calcium regulatory proteins". Biochimica et Biophysica Acta (BBA) - Proteins and Proteomics 1703 (2): 121–134. January 2005. doi:10.1016/j.bbapap.2004.09.012. PMID 15680220. https://zenodo.org/record/1258778. 
  8. 8.00 8.01 8.02 8.03 8.04 8.05 8.06 8.07 8.08 8.09 8.10 8.11 8.12 8.13 "Bacterial methionine biosynthesis". Microbiology 160 (Pt 8): 1571–1584. August 2014. doi:10.1099/mic.0.077826-0. PMID 24939187. 
  9. "Global incorporation of norleucine in place of methionine in cytochrome P450 BM-3 heme domain increases peroxygenase activity". Biotechnology and Bioengineering 83 (6): 729–734. September 2003. doi:10.1002/bit.10718. PMID 12889037. 
  10. "Norvaline and norleucine may have been more abundant protein components during early stages of cell evolution". Origins of Life and Evolution of the Biosphere 43 (4–5): 363–375. October 2013. doi:10.1007/s11084-013-9344-3. PMID 24013929. Bibcode2013OLEB...43..363A. 
  11. "Arginine as an evolutionary intruder into protein synthesis". Biochemical and Biophysical Research Communications 53 (3): 709–714. August 1973. doi:10.1016/0006-291x(73)90151-4. PMID 4731949. 
  12. "Agmatine-conjugated cytidine in a tRNA anticodon is essential for AUA decoding in archaea". Nature Chemical Biology 6 (4): 277–282. April 2010. doi:10.1038/nchembio.323. PMID 20139989. 
  13. "Codon and amino-acid specificities of a transfer RNA are both converted by a single post-transcriptional modification". Nature 336 (6195): 179–181. November 1988. doi:10.1038/336179a0. PMID 3054566. Bibcode1988Natur.336..179M. 
  14. "A novel O-phospho-L-serine sulfhydrylation reaction catalyzed by O-acetylserine sulfhydrylase from Aeropyrum pernix K1". FEBS Letters 551 (1–3): 133–138. September 2003. doi:10.1016/S0014-5793(03)00913-X. PMID 12965218. 
  15. Karlheinz Drauz; Ian Grayson; Axel Kleemann; Hans-Peter Krimmer; Wolfgang Leuchtenberger; Christoph Weckbecker (2006). "Ullmann's Encyclopedia of Industrial Chemistry". Ullmann's Encyclopedia of Industrial Chemistry. Weinheim: Wiley-VCH. doi:10.1002/14356007.a02_057.pub2. 
  16. Barger, G.; Weichselbaum, T. E. (1934). "dl-Methionine". Organic Syntheses 14: 58. http://www.orgsyn.org/demo.aspx?prep=CV2P0384. ; Collective Volume, 2, pp. 384 
  17. "Methionine". http://www.webmd.com/vitamins-supplements/ingredientmono-42-methionine.aspx?activeingredientid=42&. 
  18. "A review of methionine dependency and the role of methionine restriction in cancer growth control and life-span extension". Cancer Treatment Reviews 38 (6): 726–736. 2012. doi:10.1016/j.ctrv.2012.01.004. PMID 22342103. 
  19. "Methionine dependency and cancer treatment". Cancer Treatment Reviews 29 (6): 489–499. 2003. doi:10.1016/S0305-7372(03)00118-X. PMID 14585259. 
  20. 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. https://www.nap.edu/read/10490/chapter/12. 
  21. "Methionine metabolism in mammals". The Journal of Nutritional Biochemistry 1 (5): 228–237. May 1990. doi:10.1016/0955-2863(90)90070-2. PMID 15539209. 
  22. Palika, Liz (1996). The Consumer's Guide to Dog Food: What's in Dog Food, Why It's There and How to Choose the Best Food for Your Dog. New York: Howell Book House. ISBN 978-0-87605-467-3. 
  23. 23.0 23.1 "Amino-acid imbalance explains extension of lifespan by dietary restriction in Drosophila". Nature 462 (7276): 1061–1064. December 2009. doi:10.1038/nature08619. PMID 19956092. Bibcode2009Natur.462.1061G. 
  24. "Methionine-deficient diet extends mouse lifespan, slows immune and lens aging, alters glucose, T4, IGF-I and insulin levels, and increases hepatocyte MIF levels and stress resistance". Aging Cell 4 (3): 119–125. June 2005. doi:10.1111/j.1474-9726.2005.00152.x. PMID 15924568. .
  25. "Growth hormone signaling is necessary for lifespan extension by dietary methionine". Aging Cell 13 (6): 1019–1027. December 2014. doi:10.1111/acel.12269. PMID 25234161. 
  26. "Metabolic adaptation of short-living growth hormone transgenic mice to methionine restriction and supplementation". Annals of the New York Academy of Sciences 1418 (1): 118–136. April 2018. doi:10.1111/nyas.13687. PMID 29722030. Bibcode2018NYASA1418..118B. 
  27. "Amino-acid imbalance explains extension of lifespan by dietary restriction in Drosophila". Nature 462 (7276): 1061–1064. December 2009. doi:10.1038/nature08619. PMID 19956092. Bibcode2009Natur.462.1061G. 
  28. "Amino acid recipe could be right for long life". Science News. December 2, 2009. http://www.sciencenews.org/view/generic/id/50275/title/Amino_acid_recipe_could_be_right_for_long_life. 
  29. "Endogenous hydrogen sulfide production is essential for dietary restriction benefits". Cell 160 (1–2): 132–144. January 2015. doi:10.1016/j.cell.2014.11.048. PMID 25542313. 
  30. "Nutritional Regulation of Hepatic FGF21 by Dietary Restriction of Methionine". Frontiers in Endocrinology 12: 773975. 2021. doi:10.3389/fendo.2021.773975. PMID 34917032. 
  31. "Methionine restriction increases blood glutathione and longevity in F344 rats". FASEB Journal 8 (15): 1302–1307. December 1994. doi:10.1096/fasebj.8.15.8001743. PMID 8001743. 
  32. "Life-span extension in mice by preweaning food restriction and by methionine restriction in middle age". The Journals of Gerontology. Series A, Biological Sciences and Medical Sciences 64 (7): 711–722. July 2009. doi:10.1093/gerona/glp051. PMID 19414512. 
  33. "Methionine restriction inhibits colon carcinogenesis". Nutrition and Cancer 54 (2): 202–208. 2006. doi:10.1207/s15327914nc5402_6. PMID 16898864. 
  34. "A review of methionine dependency and the role of methionine restriction in cancer growth control and life-span extension". Cancer Treatment Reviews 38 (6): 726–736. October 2012. doi:10.1016/j.ctrv.2012.01.004. PMID 22342103. 
  35. 35.0 35.1 Haws, Spencer A.; Yu, Deyang; Ye, Cunqi; Wille, Coral K.; Nguyen, Long C.; Krautkramer, Kimberly A.; Tomasiewicz, Jay L.; Yang, Shany E. et al. (2020-03-13). "Methyl-Metabolite Depletion Elicits Adaptive Responses to Support Heterochromatin Stability and Epigenetic Persistence". Molecular Cell 78 (2): 210–223.e8. doi:10.1016/j.molcel.2020.03.004. ISSN 1097-4164. PMID 32208170. 
  36. "Effect of methionine dietary supplementation on mitochondrial oxygen radical generation and oxidative DNA damage in rat liver and heart". Journal of Bioenergetics and Biomembranes 41 (3): 309–321. June 2009. doi:10.1007/s10863-009-9229-3. PMID 19633937. 
  37. "Methionine deficiency and hepatic injury in a dietary steatohepatitis model". Digestive Diseases and Sciences 53 (3): 767–776. March 2008. doi:10.1007/s10620-007-9900-7. PMID 17710550. 
  38. "Short-term methionine deprivation improves metabolic health via sexually dimorphic, mTORC1-independent mechanisms". FASEB Journal 32 (6): 3471–3482. January 2018. doi:10.1096/fj.201701211R. PMID 29401631. 
  39. Castaño-Martinez, Teresa; Schumacher, Fabian; Schumacher, Silke; Kochlik, Bastian; Weber, Daniela; Grune, Tilman; Biemann, Ronald; McCann, Adrian et al. (2019-03-06). "Methionine restriction prevents onset of type 2 diabetes in NZO mice". The FASEB Journal 33 (6): 7092–7102. doi:10.1096/fj.201900150R. ISSN 1530-6860. PMID 30841758. 
  40. "Senile hair graying: H2O2-mediated oxidative stress affects human hair color by blunting methionine sulfoxide repair". FASEB Journal 23 (7): 2065–75. July 2009. doi:10.1096/fj.08-125435. PMID 19237503. 
  41. "Codrugs linking L-dopa and sulfur-containing antioxidants: new pharmacological tools against Parkinson's disease". Journal of Medicinal Chemistry 52 (2): 559–63. 2009. doi:10.1021/jm801266x. PMID 19093882. 
  42. "Homocysteine and cardiovascular disease". Annual Review of Medicine 49 (1): 31–62. 1998. doi:10.1146/annurev.med.49.1.31. PMID 9509248. 
  43. Grimshaw, Jane (July 25, 2011) Methionine for Dogs uses and Side Effects. critters360.com
  44. "Rules and Regulations". Federal Register 76 (49): 13501–13504. March 14, 2011. http://edocket.access.gpo.gov/2011/2011-5716.htm. 
  45. "A novel biorational pesticide: efficacy of methionine against Heraclides (Papilio) cresphontes, a surrogate of the invasive Princeps (Papilio) demoleus (Lepidoptera: Papilionidae)". Journal of Economic Entomology 104 (6): 1986–1990. December 2011. doi:10.1603/ec11132. PMID 22299361. 

External links