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{{Infobox medical condition (new)
{{Infobox medical condition (new)
| name = Hyperhomocysteinemia
| name = Hyperhomocysteinemia
| synonyms = '''Hyperhomocysteinaemia'''
| synonyms = '''Hyperhomocysteinaemia'''
| image = Plasma tHcy.svg
| image = Plasma tHcy.svg
| caption = [[Homocysteine|Total plasma homocysteine]]
| caption = [[Homocysteine|Total plasma homocysteine]]
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| types =
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'''Hyperhomocysteinemia''' is a medical condition characterized by an abnormally high level of [[homocysteine]] in the [[blood]], conventionally described as above 15&nbsp;µmol/L.<ref>{{cite journal |pmid=19491420 |year=2009 |last1=Guo |first1=H |title=Influence of folic acid on plasma homocysteine levels & arterial endothelial function in patients with unstable angina |journal=The Indian Journal of Medical Research |volume=129 |issue=3 |pages=279–84 |last2=Chi |first2=J |last3=Xing |first3=Y |last4=Wang |first4=P }}</ref>
'''Hyperhomocysteinemia''' is a medical condition characterized by an abnormally high level of [[homocysteine|total homocysteine]] (that is, including [[homocystine]] and homocysteine-cysteine disulfide) in the [[blood]], conventionally described as above 15&nbsp;μmol/L.<ref>{{cite journal |pmid=19491420 |year=2009 |last1=Guo |first1=H |title=Influence of folic acid on plasma homocysteine levels & arterial endothelial function in patients with unstable angina |journal=The Indian Journal of Medical Research |volume=129 |issue=3 |pages=279–84 |last2=Chi |first2=J |last3=Xing |first3=Y |last4=Wang |first4=P }}</ref>


As a consequence of the biochemical reactions in which homocysteine is involved, deficiencies of
As a consequence of the biochemical reactions in which homocysteine is involved, deficiencies of
[[vitamin B6|vitamin B<sub>6</sub>]], [[folic acid]] (vitamin B<sub>9</sub>), and [[Cobalamin|vitamin B<sub>12</sub>]] can lead to high homocysteine levels.<ref name="Miller-p1033-9">{{cite journal |pmid=8172087 |year=1994 |last1=Miller |first1=J. W. |title=Vitamin B-6 deficiency vs folate deficiency: Comparison of responses to methionine loading in rats |journal=The American Journal of Clinical Nutrition |volume=59 |issue=5 |pages=1033–9 |last2=Nadeau |first2=M. R. |last3=Smith |first3=D |last4=Selhub |first4=J |doi=10.1093/ajcn/59.5.1033}}</ref>
[[vitamin B6|vitamin B<sub>6</sub>]], [[folic acid]] (vitamin B<sub>9</sub>), and [[Cobalamin|vitamin B<sub>12</sub>]] can lead to high homocysteine levels.<ref name="Miller-p1033-9">{{cite journal |pmid=8172087 |year=1994 |last1=Miller |first1=J. W. |title=Vitamin B-6 deficiency vs folate deficiency: Comparison of responses to methionine loading in rats |journal=The American Journal of Clinical Nutrition |volume=59 |issue=5 |pages=1033–9 |last2=Nadeau |first2=M. R. |last3=Smith |first3=D |last4=Selhub |first4=J |doi=10.1093/ajcn/59.5.1033}}</ref> Other possible causes of hyperhomocysteinemia include genetics, excessive [[methionine]] intake, and other diseases.<ref>{{Cite journal |last=Kim |first=Jihyun |last2=Kim |first2=Hyunhee |last3=Roh |first3=Heewon |last4=Kwon |first4=Youngjoo |date=2018-04-01 |title=Causes of hyperhomocysteinemia and its pathological significance |url=http://link.springer.com/10.1007/s12272-018-1016-4 |journal=Archives of Pharmacal Research |language=en |volume=41 |issue=4 |pages=372–383 |doi=10.1007/s12272-018-1016-4 |issn=0253-6269}}</ref>


Hyperhomocysteinemia is typically managed with vitamin B6, vitamin B9 and vitamin B12 supplementation.<ref name="ExpertOpPharm2001-Coen">{{cite journal |doi=10.1517/14656566.2.9.1449 |pmid=11585023 |title=Homocysteine-lowering treatment: An overview |journal=Expert Opinion on Pharmacotherapy |volume=2 |issue=9 |pages=1449–60 |year=2005 |last1=Stehouwer |first1=Coen DA |last2=Guldener |first2=Coen van }}</ref> Hyperhomocysteinemia is a risk factor for cardiovascular disease; however, supplements of these vitamins do not improve cardiovascular disease outcomes.<ref name=Art2015 />
Hyperhomocysteinemia is typically managed with vitamin B<sub>6</sub>, vitamin B<sub>9</sub> and vitamin B<sub>12</sub> supplementation.<ref name="ExpertOpPharm2001-Coen">{{cite journal |doi=10.1517/14656566.2.9.1449 |pmid=11585023 |title=Homocysteine-lowering treatment: An overview |journal=Expert Opinion on Pharmacotherapy |volume=2 |issue=9 |pages=1449–60 |year=2005 |last1=Stehouwer |first1=Coen DA |last2=Guldener |first2=Coen van |s2cid=45945199 }}</ref> Hyperhomocysteinemia is a risk factor for cardiovascular disease; supplements of these vitamins may slightly reduce stroke outcome but not myocardial infarction, death from any cause or adverse events.<ref name=Cochrane2017>{{Cite journal |last=Martí-Carvajal |first=Arturo J |last2=Solà |first2=Ivan |last3=Lathyris |first3=Dimitrios |last4=Dayer |first4=Mark |date=2017-08-17 |editor-last=Cochrane Heart Group |title=Homocysteine-lowering interventions for preventing cardiovascular events |url=http://doi.wiley.com/10.1002/14651858.CD006612.pub5 |journal=Cochrane Database of Systematic Reviews |language=en |volume=2021 |issue=9 |doi=10.1002/14651858.CD006612.pub5 |pmc=6483699 |pmid=28816346}}</ref>


== Signs and symptoms ==
== Signs and symptoms ==
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=== Cardiovascular risks ===
=== Cardiovascular risks ===
Elevated homocysteine is a known risk factor for cardiovascular disease as well as [[thrombosis]].<ref>{{cite journal |pmid=10063987 |url=http://www.schattauer.de/index.php?id=1268&L=1&pii=th99020165&no_cache=1 |year=1999 |last1=Cattaneo |first1=Marco |title=Hyperhomocysteinemia, atherosclerosis and thrombosis |journal=Thrombosis and Haemostasis |volume=81 |issue=2 |pages=165–76 |doi=10.1055/s-0037-1614438 }}</ref> It has also been shown to be associated with [[microalbuminuria]] which is a strong indicator of the risk of future cardiovascular disease and renal dysfunction.<ref>{{cite journal |doi=10.1161/01.ATV.21.1.74 |pmid=11145936 |title=Serum Homocysteine Levels Are Associated with the Development of (Micro)albuminuria : The Hoorn Study |journal=Arteriosclerosis, Thrombosis, and Vascular Biology |volume=21 |issue=1 |pages=74–81 |year=2001 |last1=Jager |first1=A. |last2=Kostense |first2=P. J. |last3=Nijpels |first3=G. |last4=Dekker |first4=J. M. |last5=Heine |first5=R. J. |last6=Bouter |first6=L. M. |last7=Donker |first7=A. J. M. |last8=Stehouwer |first8=C. D. A. }}</ref> Homocysteine degrades and inhibits the formation of the three main structural components of [[arteries]]: [[collagen]], [[elastin]] and [[proteoglycans]]. In [[protein]]s, homocysteine permanently degrades cysteine [[disulfide bridges]] and lysine amino acid residues,<ref>{{cite journal |pmid=16702349 |year=2006 |last1=Jakubowski |first1=H |title=Pathophysiological consequences of homocysteine excess |journal=The Journal of Nutrition |volume=136 |issue=6 Suppl |pages=1741S–1749S |doi=10.1093/jn/136.6.1741S }}</ref> affecting structure and function.
Elevated homocysteine is a known risk factor for cardiovascular disease as well as [[thrombosis]].<ref>{{cite journal |pmid=10063987 |url=http://www.schattauer.de/index.php?id=1268&L=1&pii=th99020165&no_cache=1 |year=1999 |last1=Cattaneo |first1=Marco |title=Hyperhomocysteinemia, atherosclerosis and thrombosis |journal=Thrombosis and Haemostasis |volume=81 |issue=2 |pages=165–76 |doi=10.1055/s-0037-1614438 | s2cid=13228673 |access-date=2016-12-27 |archive-date=2018-07-21 |archive-url=https://web.archive.org/web/20180721145531/https://www.schattauer.de/index.php?id=1690 |url-status=dead }}</ref> It has also been shown to be associated with [[microalbuminuria]] which is a strong indicator of the risk of future cardiovascular disease and renal dysfunction.<ref>{{cite journal |doi=10.1161/01.ATV.21.1.74 |pmid=11145936 |title=Serum Homocysteine Levels Are Associated with the Development of (Micro)albuminuria : The Hoorn Study |journal=Arteriosclerosis, Thrombosis, and Vascular Biology |volume=21 |issue=1 |pages=74–81 |year=2001 |last1=Jager |first1=A. |last2=Kostense |first2=P. J. |last3=Nijpels |first3=G. |last4=Dekker |first4=J. M. |last5=Heine |first5=R. J. |last6=Bouter |first6=L. M. |last7=Donker |first7=A. J. M. |last8=Stehouwer |first8=C. D. A. |doi-access=free }}</ref> Homocysteine degrades and inhibits the formation of the three main structural components of [[arteries]]: [[collagen]], [[elastin]] and [[proteoglycans]]. In [[protein]]s, homocysteine permanently degrades cysteine [[disulfide bridges]] and lysine amino acid residues,<ref>{{cite journal |pmid=16702349 |year=2006 |last1=Jakubowski |first1=H |title=Pathophysiological consequences of homocysteine excess |journal=The Journal of Nutrition |volume=136 |issue=6 Suppl |pages=1741S–1749S |doi=10.1093/jn/136.6.1741S |doi-access=free }}</ref> affecting structure and function.


=== Neuropsychiatric illness ===
=== Neuropsychiatric illness ===
Evidence exists linking elevated homocysteine levels with [[Vascular dementia|vascular dementia]]<ref>{{Cite journal|last=McVeigh|first=Catherine|last2=Passmore|first2=Peter|date=September 2006|title=Vascular dementia: prevention and treatment|journal=Clinical Interventions in Aging|volume=1|issue=3|pages=229–235|issn=1176-9092|pmc=2695177|pmid=18046875|doi=10.2147/ciia.2006.1.3.229}}</ref> and [[Alzheimer's disease]].<ref>{{cite journal |doi=10.1016/s1474-4422(03)00438-1 |pmid=12849121 |title=Homocysteine and Alzheimer's disease |journal=The Lancet Neurology |volume=2 |issue=7 |pages=425–8 |year=2003 |last1=Morris |first1=Martha Savaria }}</ref><ref>{{cite journal |doi=10.1159/000326301 |pmid=21474939 |title=Folate and Homocysteine in the Cerebrospinal Fluid of Patients with Alzheimer's Disease or Dementia: A Case Control Study |journal=European Neurology |volume=65 |issue=5 |pages=270–8 |year=2011 |last1=Smach |first1=Mohamed Ali |last2=Jacob |first2=Nelly |last3=Golmard |first3=Jean-Louis |last4=Charfeddine |first4=Bassem |last5=Lammouchi |first5=Turkia |last6=Ben Othman |first6=Leila |last7=Dridi |first7=Hedi |last8=Bennamou |first8=Soufien |last9=Limem |first9=Khalifa }}</ref><ref>{{cite journal |doi=10.1371/journal.pone.0012244 |pmid=20838622 |pmc=2935890 |title=Homocysteine-Lowering by B Vitamins Slows the Rate of Accelerated Brain Atrophy in Mild Cognitive Impairment: A Randomized Controlled Trial |journal=PLoS ONE |volume=5 |issue=9 |pages=e12244 |year=2010 |last1=Smith |first1=A. David |last2=Smith |first2=Stephen M. |last3=De Jager |first3=Celeste A. |last4=Whitbread |first4=Philippa |last5=Johnston |first5=Carole |last6=Agacinski |first6=Grzegorz |last7=Oulhaj |first7=Abderrahim |last8=Bradley |first8=Kevin M. |last9=Jacoby |first9=Robin |last10=Refsum |first10=Helga |bibcode=2010PLoSO...512244S }}</ref> There is also evidence that elevated homocysteine levels and low levels of vitamin B6 and B12 are risk factors for [[mild cognitive impairment]] and [[dementia]].<ref name="pmid19769453">{{cite journal |doi=10.1586/ern.09.75 |pmid=19769453 |title=Homocysteine, folate and vitamin B12in neuropsychiatric diseases: Review and treatment recommendations |journal=Expert Review of Neurotherapeutics |volume=9 |issue=9 |pages=1393–412 |year=2014 |last1=Stanger |first1=Olaf |last2=Fowler |first2=Brian |last3=Piertzik |first3=Klaus |last4=Huemer |first4=Martina |last5=Haschke-Becher |first5=Elisabeth |last6=Semmler |first6=Alexander |last7=Lorenzl |first7=Stefan |last8=Linnebank |first8=Michael |url=https://www.zora.uzh.ch/id/eprint/21178/1/DACH_Zora.pdf }}</ref> Oxidative stress induced by homocysteine may also play a role in [[schizophrenia]].<ref>{{cite journal |doi=10.1007/s11064-012-0707-3 |pmid=22270909 |pmc=3321271 |title=The Oxidative Stress May be Induced by the Elevated Homocysteine in Schizophrenic Patients |journal=Neurochemical Research |volume=37 |issue=5 |pages=1057–62 |year=2012 |last1=Dietrich-Muszalska |first1=Anna |last2=Malinowska |first2=Joanna |last3=Olas |first3=Beata |last4=Głowacki |first4=Rafal |last5=Bald |first5=Edward |last6=Wachowicz |first6=Barbara |last7=Rabe-Jabłońska |first7=Jolanta }}</ref>
Evidence exists linking elevated homocysteine levels with [[vascular dementia]]<ref>{{Cite journal|last1=McVeigh|first1=Catherine|last2=Passmore|first2=Peter|date=September 2006|title=Vascular dementia: prevention and treatment|journal=Clinical Interventions in Aging|volume=1|issue=3|pages=229–235|issn=1176-9092|pmc=2695177|pmid=18046875|doi=10.2147/ciia.2006.1.3.229 |doi-access=free }}</ref> and [[Alzheimer's disease]].<ref>{{cite journal |doi=10.1016/s1474-4422(03)00438-1 |pmid=12849121 |title=Homocysteine and Alzheimer's disease |journal=The Lancet Neurology |volume=2 |issue=7 |pages=425–8 |year=2003 |last1=Morris |first1=Martha Savaria |s2cid=20443022 }}</ref><ref>{{cite journal |doi=10.1159/000326301 |pmid=21474939 |title=Folate and Homocysteine in the Cerebrospinal Fluid of Patients with Alzheimer's Disease or Dementia: A Case Control Study |journal=European Neurology |volume=65 |issue=5 |pages=270–8 |year=2011 |last1=Smach |first1=Mohamed Ali |last2=Jacob |first2=Nelly |last3=Golmard |first3=Jean-Louis |last4=Charfeddine |first4=Bassem |last5=Lammouchi |first5=Turkia |last6=Ben Othman |first6=Leila |last7=Dridi |first7=Hedi |last8=Bennamou |first8=Soufien |last9=Limem |first9=Khalifa |s2cid=7689901 }}</ref><ref>{{cite journal |doi=10.1371/journal.pone.0012244 |pmid=20838622 |pmc=2935890 |title=Homocysteine-Lowering by B Vitamins Slows the Rate of Accelerated Brain Atrophy in Mild Cognitive Impairment: A Randomized Controlled Trial |journal=PLOS ONE |volume=5 |issue=9 |pages=e12244 |year=2010 |last1=Smith |first1=A. David |last2=Smith |first2=Stephen M. |last3=De Jager |first3=Celeste A. |last4=Whitbread |first4=Philippa |last5=Johnston |first5=Carole |last6=Agacinski |first6=Grzegorz |last7=Oulhaj |first7=Abderrahim |last8=Bradley |first8=Kevin M. |last9=Jacoby |first9=Robin |last10=Refsum |first10=Helga |bibcode=2010PLoSO...512244S |doi-access=free }}</ref> There is also evidence that elevated homocysteine levels and low levels of vitamin B6 and B12 are risk factors for [[mild cognitive impairment]] and [[dementia]].<ref name="pmid19769453">{{cite journal |doi=10.1586/ern.09.75 |pmid=19769453 |title=Homocysteine, folate and vitamin B12in neuropsychiatric diseases: Review and treatment recommendations |journal=Expert Review of Neurotherapeutics |volume=9 |issue=9 |pages=1393–412 |year=2014 |last1=Stanger |first1=Olaf |last2=Fowler |first2=Brian |last3=Piertzik |first3=Klaus |last4=Huemer |first4=Martina |last5=Haschke-Becher |first5=Elisabeth |last6=Semmler |first6=Alexander |last7=Lorenzl |first7=Stefan |last8=Linnebank |first8=Michael |s2cid=13246020 |url=https://www.zora.uzh.ch/id/eprint/21178/1/DACH_Zora.pdf }}</ref> Oxidative stress induced by homocysteine may also play a role in [[schizophrenia]].<ref>{{cite journal |doi=10.1007/s11064-012-0707-3 |pmid=22270909 |pmc=3321271 |title=The Oxidative Stress May be Induced by the Elevated Homocysteine in Schizophrenic Patients |journal=Neurochemical Research |volume=37 |issue=5 |pages=1057–62 |year=2012 |last1=Dietrich-Muszalska |first1=Anna |last2=Malinowska |first2=Joanna |last3=Olas |first3=Beata |last4=Głowacki |first4=Rafal |last5=Bald |first5=Edward |last6=Wachowicz |first6=Barbara |last7=Rabe-Jabłońska |first7=Jolanta }}</ref>


=== Bone health ===
=== Bone health ===
Elevated levels of homocysteine have also been linked to increased [[Fracture (bone)|fractures]] in elderly persons. Homocysteine auto-oxidizes and reacts with reactive oxygen intermediates, damaging endothelial cells and increasing the risk of [[thrombus]] formation.<ref>{{cite journal |doi=10.1056/NEJMoa032739 |pmid=15141042 |title=Homocysteine as a Predictive Factor for Hip Fracture in Older Persons |journal=New England Journal of Medicine |volume=350 |issue=20 |pages=2042–9 |year=2004 |last1=McLean |first1=Robert R. |last2=Jacques |first2=Paul F. |last3=Selhub |first3=Jacob |last4=Tucker |first4=Katherine L. |last5=Samelson |first5=Elizabeth J. |last6=Broe |first6=Kerry E. |last7=Hannan |first7=Marian T. |last8=Cupples |first8=L. Adrienne |last9=Kiel |first9=Douglas P. |url=https://semanticscholar.org/paper/a986ab209653c58cf890e940dd7777992f2f84c7 }}</ref><ref>{{cite journal |doi=10.1056/NEJMoa032546 |pmid=15141041 |title=Homocysteine Levels and the Risk of Osteoporotic Fracture |journal=New England Journal of Medicine |volume=350 |issue=20 |pages=2033–41 |year=2004 |last1=Van Meurs |first1=Joyce B.J. |last2=Dhonukshe-Rutten |first2=Rosalie A.M. |last3=Pluijm |first3=Saskia M.F. |last4=Van Der Klift |first4=Marjolein |last5=De Jonge |first5=Robert |last6=Lindemans |first6=Jan |last7=De Groot |first7=Lisette C.P.G.M. |last8=Hofman |first8=Albert |last9=Witteman |first9=Jacqueline C.M. |last10=Van Leeuwen |first10=Johannes P.T.M. |last11=Breteler |first11=Monique M.B. |last12=Lips |first12=Paul |last13=Pols |first13=Huibert A.P. |last14=Uitterlinden |first14=André G. |hdl=1765/8452 |url=http://repub.eur.nl/pub/8452 }}</ref>
Elevated levels of homocysteine have also been linked to increased [[Fracture (bone)|fractures]] in elderly persons. Homocysteine auto-oxidizes and reacts with reactive oxygen intermediates, damaging endothelial cells and increasing the risk of [[thrombus]] formation.<ref>{{cite journal |doi=10.1056/NEJMoa032739 |pmid=15141042 |title=Homocysteine as a Predictive Factor for Hip Fracture in Older Persons |journal=New England Journal of Medicine |volume=350 |issue=20 |pages=2042–9 |year=2004 |last1=McLean |first1=Robert R. |last2=Jacques |first2=Paul F. |last3=Selhub |first3=Jacob |last4=Tucker |first4=Katherine L. |last5=Samelson |first5=Elizabeth J. |last6=Broe |first6=Kerry E. |last7=Hannan |first7=Marian T. |last8=Cupples |first8=L. Adrienne |last9=Kiel |first9=Douglas P. |s2cid=22853996 |doi-access=free }}</ref><ref>{{cite journal |doi=10.1056/NEJMoa032546 |pmid=15141041 |title=Homocysteine Levels and the Risk of Osteoporotic Fracture |journal=New England Journal of Medicine |volume=350 |issue=20 |pages=2033–41 |year=2004 |last1=Van Meurs |first1=Joyce B.J. |last2=Dhonukshe-Rutten |first2=Rosalie A.M. |last3=Pluijm |first3=Saskia M.F. |last4=Van Der Klift |first4=Marjolein |last5=De Jonge |first5=Robert |last6=Lindemans |first6=Jan |last7=De Groot |first7=Lisette C.P.G.M. |last8=Hofman |first8=Albert |last9=Witteman |first9=Jacqueline C.M. |last10=Van Leeuwen |first10=Johannes P.T.M. |last11=Breteler |first11=Monique M.B. |last12=Lips |first12=Paul |last13=Pols |first13=Huibert A.P. |last14=Uitterlinden |first14=André G. |hdl=1765/8452 |url=http://repub.eur.nl/pub/8452 |hdl-access=free }}</ref>


=== Ectopia lentis ===
=== Ectopia lentis ===
Homocystinuria is the second most common cause of heritable [[ectopia lentis]]. Homocystinuria is an autosomal recessive metabolic disorder most often caused by a near absence of cystathionine b-synthetase. It is associated with intellectual disability, osteoporosis, chest deformities, and increased risk of thrombotic episodes. Lens dislocation occurs in 90% of patients, and is thought to be due to decreased zonular integrity due to the enzymatic defect. Lens dislocation in homocystinuria is usually bilateral and in 60% of cases occurs in the inferior or nasal direction.
[[Homocystinuria]] is the second most common cause of heritable [[ectopia lentis]]. Homocystinuria is an autosomal recessive metabolic disorder most often caused by a near absence of cystathionine b-synthetase. It is associated with intellectual disability, osteoporosis, chest deformities, and increased risk of thrombotic episodes. Lens dislocation occurs in 90% of patients, and is thought to be due to decreased zonular integrity due to the enzymatic defect. Lens dislocation in homocystinuria is usually bilateral and in 60% of cases occurs in the inferior or nasal direction.{{citation needed|date=June 2022}}


== Causes ==
== Causes ==
=== Vitamin deficiency ===
Deficiencies of vitamins B6, B9, and B12 can lead to high homocysteine levels.<ref name="Miller-p1033-9" /> [[Vitamin B12]], or cobalamin, acts as a cofactor for the enzyme [[methionine synthase]] (which forms part of the [[S-adenosylmethionine]] (SAM) biosynthesis and regeneration cycle). Vitamin B12 deficiency prevents the 5-methyltetrahydrofolate (5-MTHF) form of folate from being converted into THF due to the "methyl trap".<ref>{{cite journal |doi=10.1074/jbc.M410818200 |pmid=15496403 |title=A Mathematical Model of the Folate Cycle: new insights into folate homeostasis |journal=Journal of Biological Chemistry |volume=279 |issue=53 |pages=55008–16 |year=2004 |last1=Nijhout |first1=H. Frederik |last2=Reed |first2=Michael C. |last3=Budu |first3=Paula |last4=Ulrich |first4=Cornelia M. }}</ref> This disrupts the [[folate]] pathway and leads to an increase in homocysteine which damages cells (for example, damage to endothelial cells can result in increased risk of thrombosis).
Deficiencies of vitamins B<sub>6</sub>, B<sub>9</sub> and B<sub>12</sub> can lead to high homocysteine levels.<ref name="Miller-p1033-9" /> Vitamin B<sub>12</sub> acts as a cofactor for the enzyme [[methionine synthase]] (which forms part of the [[S-adenosylmethionine]] (SAM) biosynthesis and regeneration cycle). Vitamin B<sub>12</sub> deficiency prevents the 5-methyltetrahydrofolate (5-MTHF) form of folate from being converted into THF due to the "methyl trap".<ref>{{cite journal |doi=10.1074/jbc.M410818200 |pmid=15496403 |title=A Mathematical Model of the Folate Cycle: new insights into folate homeostasis |journal=Journal of Biological Chemistry |volume=279 |issue=53 |pages=55008–16 |year=2004 |last1=Nijhout |first1=H. Frederik |last2=Reed |first2=Michael C. |last3=Budu |first3=Paula |last4=Ulrich |first4=Cornelia M. |doi-access=free }}</ref> This disrupts the [[folate]] pathway and leads to an increase in homocysteine which damages cells (for example, damage to endothelial cells can result in increased risk of thrombosis).


=== Alcohol ===
Chronic consumption of alcohol may also result in increased plasma levels of homocysteine.<ref>{{cite journal |doi=10.1093/alcalc/36.3.189 |pmid=11373253 |title=Moderate alcohol consumption in social drinkers raises plasma homocysteine levels: A contradiction to the 'French Paradox'? |journal=Alcohol and Alcoholism |volume=36 |issue=3 |pages=189–92 |year=2001 |last1=Bleich |first1=S. |last2=Bleich |first2=K |last3=Kropp |first3=S |last4=Bittermann |first4=H. J. |last5=Degner |first5=D |last6=Sperling |first6=W |last7=Rüther |first7=E |last8=Kornhuber |first8=J }}</ref><ref>{{cite journal |doi=10.1097/01.alc.0000156083.91214.59 |pmid=15770107 |title=Evidence of Increased Homocysteine Levels in Alcoholism: The Franconian Alcoholism Research Studies (FARS) |journal=Alcoholism: Clinical & Experimental Research |volume=29 |issue=3 |pages=334–6 |year=2005 |last1=Bleich |first1=Stefan |last2=Carl |first2=Marco |last3=Bayerlein |first3=Kristina |last4=Reulbach |first4=Udo |last5=Biermann |first5=Teresa |last6=Hillemacher |first6=Thomas |last7=b??Nsch |first7=Dominikus |last8=Kornhuber |first8=Johannes }}</ref>
Chronic consumption of alcohol may also result in increased plasma levels of homocysteine.<ref>{{cite journal |doi=10.1093/alcalc/36.3.189 |pmid=11373253 |title=Moderate alcohol consumption in social drinkers raises plasma homocysteine levels: A contradiction to the 'French Paradox'? |journal=Alcohol and Alcoholism |volume=36 |issue=3 |pages=189–92 |year=2001 |last1=Bleich |first1=S. |last2=Bleich |first2=K |last3=Kropp |first3=S |last4=Bittermann |first4=H. J. |last5=Degner |first5=D |last6=Sperling |first6=W |last7=Rüther |first7=E |last8=Kornhuber |first8=J |doi-access=free }}</ref><ref>{{cite journal |doi=10.1097/01.alc.0000156083.91214.59 |pmid=15770107 |title=Evidence of Increased Homocysteine Levels in Alcoholism: The Franconian Alcoholism Research Studies (FARS) |journal=Alcoholism: Clinical & Experimental Research |volume=29 |issue=3 |pages=334–6 |year=2005 |last1=Bleich |first1=Stefan |last2=Carl |first2=Marco |last3=Bayerlein |first3=Kristina |last4=Reulbach |first4=Udo |last5=Biermann |first5=Teresa |last6=Hillemacher |first6=Thomas |last7=b??Nsch |first7=Dominikus |last8=Kornhuber |first8=Johannes }}</ref>

=== Tobacco ===
Smokeless tobacco is implicated as risk factor for hyperhomocysteinemia.<ref name="pmid24376761">{{cite journal |vauthors=Iqbal MP, Yakub M |title=Smokeless tobacco use: a risk factor for hyperhomocysteinemia in a Pakistani population |journal=[[PLOS ONE]] |volume=8 |issue=12 |pages=e83826 |date=2013 |pmid=24376761 |pmc=3871626 |doi=10.1371/journal.pone.0083826 |bibcode=2013PLoSO...883826I |url=|doi-access=free }}</ref> Smoking also causes hyperhomocysteinemia<ref name="pmid21143017">{{cite journal |vauthors=Haj Mouhamed D, Ezzaher A, Neffati F, Douki W, Najjar MF |title=Effect of cigarette smoking on plasma homocysteine concentrations |journal=[[Clinical Chemistry and Laboratory Medicine]] |volume=49 |issue=3 |pages=479–83 |date=March 2011 |pmid=21143017 |doi=10.1515/CCLM.2011.062 |s2cid=34110392 |url=}}</ref>


=== Genetic ===
=== Genetic ===
Homocysteine is a non-protein amino acid, synthesized from [[methionine]] and either recycled back into methionine or converted into [[cysteine]] with the aid of the B-group vitamins.
Homocysteine is a non-protein amino acid, synthesized from [[methionine]] and either recycled back into methionine or converted into [[cysteine]] with the aid of the B-group vitamins.
* About 50% of homocysteine {{Citation needed|date=May 2014}} is converted back to methionine by [[remethylation]] via the [[methionine synthase]] major pathway. This requires [[5-methyltetrahydrofolate|active folate]] and vitamin B<sub>12</sub>, in order to donate a methyl group. Active folate is known as 5-methyltetrahydrofolate (5-MTHF).

* About 50% of homocysteine {{Citation needed|date=May 2014}} is converted back to methionine by remethylation via the [[methionine synthase]] major pathway. This requires [[5-methyltetrahydrofolate|active folate]] and vitamin B12, in order to donate a methyl group. Active folate is known as 5-methyltetrahydrofolate (5-MTHF).
* Another pathway for the conversion of homocysteine back to methionine also exists, involving methylation with [[trimethylglycine]] (also called betaine or abbreviated to TMG) as a methyl donor.
* Another pathway for the conversion of homocysteine back to methionine also exists, involving methylation with [[trimethylglycine]] (also called betaine or abbreviated to TMG) as a methyl donor.
* The remaining homocysteine is transsulfurated to cysteine, with vitamin B6 as the co-factor.
* The remaining homocysteine is transsulfurated to cysteine, with vitamin B6 as the co-factor.


Genetic defects in [[MTHFR|5-MTHF reductase]] can consequently lead to hyperhomocysteinemia. The most common [[polymorphism (biology)|polymorphisms]] are known as MTHFR C677T and MTR A2756G.<ref>{{cite journal |doi=10.1186/1475-2891-11-2 |pmid=22230384 |pmc=3274435 |title=MTHFR C677T and MTR A2756G polymorphisms and the homocysteine lowering efficacy of different doses of folic acid in hypertensive Chinese adults |journal=Nutrition Journal |volume=11 |pages=2 |year=2012 |last1=Qin |first1=Xianhui |last2=Li |first2=Jianping |last3=Cui |first3=Yimin |last4=Liu |first4=Zeyuan |last5=Zhao |first5=Zhigang |last6=Ge |first6=Junbo |last7=Guan |first7=Deming |last8=Hu |first8=Jian |last9=Wang |first9=Yanni |last10=Zhang |first10=Fumin |last11=Xu |first11=Xin |last12=Wang |first12=Xiaobin |last13=Xu |first13=Xiping |last14=Huo |first14=Yong }}</ref><ref>{{cite journal |doi=10.1371/journal.pone.0033222 |pmid=22470444 |pmc=3310006 |title=Polymorphisms in MTHFR, MS and CBS Genes and Homocysteine Levels in a Pakistani Population |journal=PLoS ONE |volume=7 |issue=3 |pages=e33222 |year=2012 |last1=Yakub |first1=Mohsin |last2=Moti |first2=Naushad |last3=Parveen |first3=Siddiqa |last4=Chaudhry |first4=Bushra |last5=Azam |first5=Iqbal |last6=Iqbal |first6=Mohammad Perwaiz |bibcode=2012PLoSO...733222Y }}</ref> These polymorphisms occur in about 10% of the world's population.{{Citation needed|date=June 2013}} Elevations of homocysteine can also occur in the rare [[genetics|hereditary]] disease [[homocystinuria]].
Genetic defects in [[MTHFR|5-MTHF reductase]] can consequently lead to hyperhomocysteinemia. The most common [[polymorphism (biology)|polymorphisms]] are known as MTHFR C677T and MTR A2756G.<ref>{{cite journal |doi=10.1186/1475-2891-11-2 |pmid=22230384 |pmc=3274435 |title=MTHFR C677T and MTR A2756G polymorphisms and the homocysteine lowering efficacy of different doses of folic acid in hypertensive Chinese adults |journal=Nutrition Journal |volume=11 |pages=2 |year=2012 |last1=Qin |first1=Xianhui |last2=Li |first2=Jianping |last3=Cui |first3=Yimin |last4=Liu |first4=Zeyuan |last5=Zhao |first5=Zhigang |last6=Ge |first6=Junbo |last7=Guan |first7=Deming |last8=Hu |first8=Jian |last9=Wang |first9=Yanni |last10=Zhang |first10=Fumin |last11=Xu |first11=Xin |last12=Wang |first12=Xiaobin |last13=Xu |first13=Xiping |last14=Huo |first14=Yong |doi-access=free }}</ref><ref>{{cite journal |doi=10.1371/journal.pone.0033222 |pmid=22470444 |pmc=3310006 |title=Polymorphisms in MTHFR, MS and CBS Genes and Homocysteine Levels in a Pakistani Population |journal=PLOS ONE |volume=7 |issue=3 |pages=e33222 |year=2012 |last1=Yakub |first1=Mohsin |last2=Moti |first2=Naushad |last3=Parveen |first3=Siddiqa |last4=Chaudhry |first4=Bushra |last5=Azam |first5=Iqbal |last6=Iqbal |first6=Mohammad Perwaiz |bibcode=2012PLoSO...733222Y |doi-access=free }}</ref> The homozigote mutation G;G also called C;C (it is equivalent) occurs in about 10% of the population of european ethnicity (white caucasians).<ref>https://www.snpedia.com/index.php/rs1801131 consulted 30.10.2023</ref> Elevations of homocysteine can also occur in the rare [[genetics|hereditary]] disease [[homocystinuria]].


== Diagnosis ==
== Diagnosis ==
A blood test can be performed to quantify total homocysteine concentration in the plasma, of which approximately 80% is generally protein-bound. Classification of hyperhomocysteinemia is defined with respect to serum concentration as follows:
A blood test can be performed to quantify total homocysteine concentration in the plasma, of which approximately 80% is generally protein-bound. Classification of hyperhomocysteinemia is defined with respect to serum concentration as follows:{{citation needed|date=June 2022}}
* Moderate: 15–30 nmol/mL (or µmol/L)
* Moderate: 15–30 nmol/mL (or μmol/L)
* Intermediate: 30–100 nmol/mL
* Intermediate: 30–100 nmol/mL
* Severe: > 100 nmol/mL
* Severe: > 100 nmol/mL
If total homocysteine concentration is not found to be elevated, but clinical suspicion is still high, an oral methionine loading challenge several hours prior to quantification of homocysteine concentration may be used to increased sensitivity for marginal abnormalities of homocysteine metabolism.<ref>{{Cite journal|last=Kang|first=S. S.|last2=Wong|first2=P. W.|date=1996-01-26|title=Genetic and nongenetic factors for moderate hyperhomocyst(e)inemia|journal=Atherosclerosis|volume=119|issue=2|pages=135–138|issn=0021-9150|pmid=8808490|doi=10.1016/0021-9150(95)05648-3}}</ref>
If total homocysteine concentration is not found to be elevated, but clinical suspicion is still high, an oral methionine loading challenge several hours prior to quantification of homocysteine concentration may be used to increased sensitivity for marginal abnormalities of homocysteine metabolism.<ref>{{Cite journal|last1=Kang|first1=S. S.|last2=Wong|first2=P. W.|date=1996-01-26|title=Genetic and nongenetic factors for moderate hyperhomocyst(e)inemia|journal=Atherosclerosis|volume=119|issue=2|pages=135–138|issn=0021-9150|pmid=8808490|doi=10.1016/0021-9150(95)05648-3}}</ref>


Fasting for 10 hours is sometimes recommended prior to measurement of homocysteine levels, but this may not be necessary for diagnostic yield.<ref>{{Cite journal|last=Fokkema|first=M. Rebecca|last2=Gilissen|first2=Marleen F.|last3=Doormaal|first3=Jasper J. van|last4=Volmer|first4=Marcel|last5=Kema|first5=Ido P.|last6=Muskiet|first6=Frits A. J.|date=2003-05-01|title=Fasting vs Nonfasting Plasma Homocysteine Concentrations for Diagnosis of Hyperhomocysteinemia|journal=Clinical Chemistry|language=en|volume=49|issue=5|pages=818–821|doi=10.1373/49.5.818|issn=0009-9147|pmid=12709379}}</ref>
Fasting for 10 hours is sometimes recommended prior to measurement of homocysteine levels, but this may not be necessary for diagnostic yield.<ref>{{Cite journal|last1=Fokkema|first1=M. Rebecca|last2=Gilissen|first2=Marleen F.|last3=Doormaal|first3=Jasper J. van|last4=Volmer|first4=Marcel|last5=Kema|first5=Ido P.|last6=Muskiet|first6=Frits A. J.|date=2003-05-01|title=Fasting vs Nonfasting Plasma Homocysteine Concentrations for Diagnosis of Hyperhomocysteinemia|journal=Clinical Chemistry|language=en|volume=49|issue=5|pages=818–821|doi=10.1373/49.5.818|issn=0009-9147|pmid=12709379|doi-access=free}}</ref>


== Treatment ==
== Treatment ==
Vitamins B<sub>6</sub>, B<sub>9</sub>, or B<sub>12</sub> supplements (alone or combined) lower homocysteine level and might slightly reduce the risk of stroke but not of myocardial infarction compared to standard care or placebo in clinical trials.<ref name=Cochrane2017/> When combined with medicine to reduce blood pressure ([[Antihypertensive drug|antihypertensive]] drugs), it is not clear if treatments that lower homocysteine can help prevent a stroke in some people.<ref name=Cochrane2017/> Hypotheses have been offered to address the failure of homocysteine-lowering therapies to reduce cardiovascular events. When [[folic acid]] is given as a supplement, it may increase the build-up of [[atherosclerosis|arterial plaque]]. A second hypothesis involves the [[methylation]] of genes in vascular cells by folic acid and vitamin B<sub>12</sub>, which may also accelerate plaque growth. Finally, altered methylation may catalyse l-arginine to asymmetric dimethylarginine, which is known to increase the risk of vascular disease.<ref>{{cite journal|last=Watson|first=KE|title=Lowering levels of lipids and homocysteine.|journal=Reviews in Cardiovascular Medicine|date=Fall 2006|volume=7|issue=4|pages=248–50|pmid=17224870}}</ref>
Vitamins B6, B9, or B12 supplements, while they lower homocysteine level do not change the risk of heart disease, stroke, or death.<ref name=Art2015>{{cite journal|first1=Arturo J.|last1=Martí-Carvajal|first2=Ivan|last2=Solà|first3=Dimitrios|last3=Lathyris|title=Homocysteine-lowering interventions for preventing cardiovascular events|journal=The Cochrane Database of Systematic Reviews|date=15 January 2015|issn=1469-493X|pages=CD006612|volume=1|pmid=25590290|pmc=4164174|doi=10.1002/14651858.CD006612.pub4|editor1-last=Martí-Carvajal|editor1-first=Arturo J}}</ref>{{Update inline|reason=Updated version https://www.ncbi.nlm.nih.gov/pubmed/28816346|date = July 2018}} This also applies to people with [[kidney disease]] on [[dialysis]].<ref>{{cite journal|first1=Sagar U.|last1=Nigwekar|first2=Amy|last2=Kang|first3=Sophia|last3=Zoungas|first4=Alan|last4=Cass|title=Interventions for lowering plasma homocysteine levels in dialysis patients|journal=The Cochrane Database of Systematic Reviews|date=31 May 2016|issn=1469-493X|pages=CD004683|issue=5|pmid=27243372|doi=10.1002/14651858.CD004683.pub4|first5=Martin P.|last5=Gallagher|first6=Satyarth|last6=Kulshrestha|first7=Sankar D.|last7=Navaneethan|first8=Vlado|last8=Perkovic|first9=Giovanni F. M.|last9=Strippoli|first10=Meg J.|last10=Jardine}}</ref>

Hypotheses have been offered to address the failure of homocysteine-lowering therapies to reduce cardiovascular events. When [[folic acid]] is given as a supplement, it may increase the build-up of [[atherosclerosis|arterial plaque]]. A second hypothesis involves the [[methylation]] of genes in vascular cells by folic acid and vitamin B12, which may also accelerate plaque growth. Finally, altered methylation may catalyse l-arginine to asymmetric dimethylarginine, which is known to increase the risk of vascular disease.<ref>{{cite journal|last=Watson|first=KE|title=Lowering levels of lipids and homocysteine.|journal=Reviews in Cardiovascular Medicine|date=Fall 2006|volume=7|issue=4|pages=248–50|pmid=17224870}}</ref>


== See also ==
== See also ==
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== External links ==
== External links ==
{{Medical resources
{{Medical resources
| DiseasesDB = 29853
| DiseasesDB = 29853
| ICD10 =
| ICD10 =
| ICD9 = {{ICD9|270.4}}
| ICD9 = {{ICD9|270.4}}
| ICDO =
| ICDO =
| OMIM =
| OMIM =
| MedlinePlus =
| MedlinePlus =
| eMedicineSubj = neuro
| eMedicineSubj = neuro
| eMedicineTopic = 578
| eMedicineTopic = 578
| MeshID =
| MeshID =
| SNOMED CT = 419503008
}}
}}

{{Amino acid metabolic pathology}}
{{Amino acid metabolic pathology}}
{{Authority control}}


[[Category:Amino acid metabolism disorders]]
[[Category:Amino acid metabolism disorders]]

Latest revision as of 15:21, 11 April 2024

Hyperhomocysteinemia
Other namesHyperhomocysteinaemia
Total plasma homocysteine
SpecialtyNutrition, medical genetics, endocrinology Edit this on Wikidata

Hyperhomocysteinemia is a medical condition characterized by an abnormally high level of total homocysteine (that is, including homocystine and homocysteine-cysteine disulfide) in the blood, conventionally described as above 15 μmol/L.[1]

As a consequence of the biochemical reactions in which homocysteine is involved, deficiencies of vitamin B6, folic acid (vitamin B9), and vitamin B12 can lead to high homocysteine levels.[2] Other possible causes of hyperhomocysteinemia include genetics, excessive methionine intake, and other diseases.[3]

Hyperhomocysteinemia is typically managed with vitamin B6, vitamin B9 and vitamin B12 supplementation.[4] Hyperhomocysteinemia is a risk factor for cardiovascular disease; supplements of these vitamins may slightly reduce stroke outcome but not myocardial infarction, death from any cause or adverse events.[5]

Signs and symptoms[edit]

Elevated levels of homocysteine have been associated with a number of disease states.

Cardiovascular risks[edit]

Elevated homocysteine is a known risk factor for cardiovascular disease as well as thrombosis.[6] It has also been shown to be associated with microalbuminuria which is a strong indicator of the risk of future cardiovascular disease and renal dysfunction.[7] Homocysteine degrades and inhibits the formation of the three main structural components of arteries: collagen, elastin and proteoglycans. In proteins, homocysteine permanently degrades cysteine disulfide bridges and lysine amino acid residues,[8] affecting structure and function.

Neuropsychiatric illness[edit]

Evidence exists linking elevated homocysteine levels with vascular dementia[9] and Alzheimer's disease.[10][11][12] There is also evidence that elevated homocysteine levels and low levels of vitamin B6 and B12 are risk factors for mild cognitive impairment and dementia.[13] Oxidative stress induced by homocysteine may also play a role in schizophrenia.[14]

Bone health[edit]

Elevated levels of homocysteine have also been linked to increased fractures in elderly persons. Homocysteine auto-oxidizes and reacts with reactive oxygen intermediates, damaging endothelial cells and increasing the risk of thrombus formation.[15][16]

Ectopia lentis[edit]

Homocystinuria is the second most common cause of heritable ectopia lentis. Homocystinuria is an autosomal recessive metabolic disorder most often caused by a near absence of cystathionine b-synthetase. It is associated with intellectual disability, osteoporosis, chest deformities, and increased risk of thrombotic episodes. Lens dislocation occurs in 90% of patients, and is thought to be due to decreased zonular integrity due to the enzymatic defect. Lens dislocation in homocystinuria is usually bilateral and in 60% of cases occurs in the inferior or nasal direction.[citation needed]

Causes[edit]

Vitamin deficiency[edit]

Deficiencies of vitamins B6, B9 and B12 can lead to high homocysteine levels.[2] Vitamin B12 acts as a cofactor for the enzyme methionine synthase (which forms part of the S-adenosylmethionine (SAM) biosynthesis and regeneration cycle). Vitamin B12 deficiency prevents the 5-methyltetrahydrofolate (5-MTHF) form of folate from being converted into THF due to the "methyl trap".[17] This disrupts the folate pathway and leads to an increase in homocysteine which damages cells (for example, damage to endothelial cells can result in increased risk of thrombosis).

Alcohol[edit]

Chronic consumption of alcohol may also result in increased plasma levels of homocysteine.[18][19]

Tobacco[edit]

Smokeless tobacco is implicated as risk factor for hyperhomocysteinemia.[20] Smoking also causes hyperhomocysteinemia[21]

Genetic[edit]

Homocysteine is a non-protein amino acid, synthesized from methionine and either recycled back into methionine or converted into cysteine with the aid of the B-group vitamins.

  • About 50% of homocysteine [citation needed] is converted back to methionine by remethylation via the methionine synthase major pathway. This requires active folate and vitamin B12, in order to donate a methyl group. Active folate is known as 5-methyltetrahydrofolate (5-MTHF).
  • Another pathway for the conversion of homocysteine back to methionine also exists, involving methylation with trimethylglycine (also called betaine or abbreviated to TMG) as a methyl donor.
  • The remaining homocysteine is transsulfurated to cysteine, with vitamin B6 as the co-factor.

Genetic defects in 5-MTHF reductase can consequently lead to hyperhomocysteinemia. The most common polymorphisms are known as MTHFR C677T and MTR A2756G.[22][23] The homozigote mutation G;G also called C;C (it is equivalent) occurs in about 10% of the population of european ethnicity (white caucasians).[24] Elevations of homocysteine can also occur in the rare hereditary disease homocystinuria.

Diagnosis[edit]

A blood test can be performed to quantify total homocysteine concentration in the plasma, of which approximately 80% is generally protein-bound. Classification of hyperhomocysteinemia is defined with respect to serum concentration as follows:[citation needed]

  • Moderate: 15–30 nmol/mL (or μmol/L)
  • Intermediate: 30–100 nmol/mL
  • Severe: > 100 nmol/mL

If total homocysteine concentration is not found to be elevated, but clinical suspicion is still high, an oral methionine loading challenge several hours prior to quantification of homocysteine concentration may be used to increased sensitivity for marginal abnormalities of homocysteine metabolism.[25]

Fasting for 10 hours is sometimes recommended prior to measurement of homocysteine levels, but this may not be necessary for diagnostic yield.[26]

Treatment[edit]

Vitamins B6, B9, or B12 supplements (alone or combined) lower homocysteine level and might slightly reduce the risk of stroke but not of myocardial infarction compared to standard care or placebo in clinical trials.[5] When combined with medicine to reduce blood pressure (antihypertensive drugs), it is not clear if treatments that lower homocysteine can help prevent a stroke in some people.[5] Hypotheses have been offered to address the failure of homocysteine-lowering therapies to reduce cardiovascular events. When folic acid is given as a supplement, it may increase the build-up of arterial plaque. A second hypothesis involves the methylation of genes in vascular cells by folic acid and vitamin B12, which may also accelerate plaque growth. Finally, altered methylation may catalyse l-arginine to asymmetric dimethylarginine, which is known to increase the risk of vascular disease.[27]

See also[edit]

References[edit]

  1. ^ Guo, H; Chi, J; Xing, Y; Wang, P (2009). "Influence of folic acid on plasma homocysteine levels & arterial endothelial function in patients with unstable angina". The Indian Journal of Medical Research. 129 (3): 279–84. PMID 19491420.
  2. ^ a b Miller, J. W.; Nadeau, M. R.; Smith, D; Selhub, J (1994). "Vitamin B-6 deficiency vs folate deficiency: Comparison of responses to methionine loading in rats". The American Journal of Clinical Nutrition. 59 (5): 1033–9. doi:10.1093/ajcn/59.5.1033. PMID 8172087.
  3. ^ Kim, Jihyun; Kim, Hyunhee; Roh, Heewon; Kwon, Youngjoo (2018-04-01). "Causes of hyperhomocysteinemia and its pathological significance". Archives of Pharmacal Research. 41 (4): 372–383. doi:10.1007/s12272-018-1016-4. ISSN 0253-6269.
  4. ^ Stehouwer, Coen DA; Guldener, Coen van (2005). "Homocysteine-lowering treatment: An overview". Expert Opinion on Pharmacotherapy. 2 (9): 1449–60. doi:10.1517/14656566.2.9.1449. PMID 11585023. S2CID 45945199.
  5. ^ a b c Martí-Carvajal, Arturo J; Solà, Ivan; Lathyris, Dimitrios; Dayer, Mark (2017-08-17). Cochrane Heart Group (ed.). "Homocysteine-lowering interventions for preventing cardiovascular events". Cochrane Database of Systematic Reviews. 2021 (9). doi:10.1002/14651858.CD006612.pub5. PMC 6483699. PMID 28816346.
  6. ^ Cattaneo, Marco (1999). "Hyperhomocysteinemia, atherosclerosis and thrombosis". Thrombosis and Haemostasis. 81 (2): 165–76. doi:10.1055/s-0037-1614438. PMID 10063987. S2CID 13228673. Archived from the original on 2018-07-21. Retrieved 2016-12-27.
  7. ^ Jager, A.; Kostense, P. J.; Nijpels, G.; Dekker, J. M.; Heine, R. J.; Bouter, L. M.; Donker, A. J. M.; Stehouwer, C. D. A. (2001). "Serum Homocysteine Levels Are Associated with the Development of (Micro)albuminuria : The Hoorn Study". Arteriosclerosis, Thrombosis, and Vascular Biology. 21 (1): 74–81. doi:10.1161/01.ATV.21.1.74. PMID 11145936.
  8. ^ Jakubowski, H (2006). "Pathophysiological consequences of homocysteine excess". The Journal of Nutrition. 136 (6 Suppl): 1741S–1749S. doi:10.1093/jn/136.6.1741S. PMID 16702349.
  9. ^ McVeigh, Catherine; Passmore, Peter (September 2006). "Vascular dementia: prevention and treatment". Clinical Interventions in Aging. 1 (3): 229–235. doi:10.2147/ciia.2006.1.3.229. ISSN 1176-9092. PMC 2695177. PMID 18046875.
  10. ^ Morris, Martha Savaria (2003). "Homocysteine and Alzheimer's disease". The Lancet Neurology. 2 (7): 425–8. doi:10.1016/s1474-4422(03)00438-1. PMID 12849121. S2CID 20443022.
  11. ^ Smach, Mohamed Ali; Jacob, Nelly; Golmard, Jean-Louis; Charfeddine, Bassem; Lammouchi, Turkia; Ben Othman, Leila; Dridi, Hedi; Bennamou, Soufien; Limem, Khalifa (2011). "Folate and Homocysteine in the Cerebrospinal Fluid of Patients with Alzheimer's Disease or Dementia: A Case Control Study". European Neurology. 65 (5): 270–8. doi:10.1159/000326301. PMID 21474939. S2CID 7689901.
  12. ^ Smith, A. David; Smith, Stephen M.; De Jager, Celeste A.; Whitbread, Philippa; Johnston, Carole; Agacinski, Grzegorz; Oulhaj, Abderrahim; Bradley, Kevin M.; Jacoby, Robin; Refsum, Helga (2010). "Homocysteine-Lowering by B Vitamins Slows the Rate of Accelerated Brain Atrophy in Mild Cognitive Impairment: A Randomized Controlled Trial". PLOS ONE. 5 (9): e12244. Bibcode:2010PLoSO...512244S. doi:10.1371/journal.pone.0012244. PMC 2935890. PMID 20838622.
  13. ^ Stanger, Olaf; Fowler, Brian; Piertzik, Klaus; Huemer, Martina; Haschke-Becher, Elisabeth; Semmler, Alexander; Lorenzl, Stefan; Linnebank, Michael (2014). "Homocysteine, folate and vitamin B12in neuropsychiatric diseases: Review and treatment recommendations" (PDF). Expert Review of Neurotherapeutics. 9 (9): 1393–412. doi:10.1586/ern.09.75. PMID 19769453. S2CID 13246020.
  14. ^ Dietrich-Muszalska, Anna; Malinowska, Joanna; Olas, Beata; Głowacki, Rafal; Bald, Edward; Wachowicz, Barbara; Rabe-Jabłońska, Jolanta (2012). "The Oxidative Stress May be Induced by the Elevated Homocysteine in Schizophrenic Patients". Neurochemical Research. 37 (5): 1057–62. doi:10.1007/s11064-012-0707-3. PMC 3321271. PMID 22270909.
  15. ^ McLean, Robert R.; Jacques, Paul F.; Selhub, Jacob; Tucker, Katherine L.; Samelson, Elizabeth J.; Broe, Kerry E.; Hannan, Marian T.; Cupples, L. Adrienne; Kiel, Douglas P. (2004). "Homocysteine as a Predictive Factor for Hip Fracture in Older Persons". New England Journal of Medicine. 350 (20): 2042–9. doi:10.1056/NEJMoa032739. PMID 15141042. S2CID 22853996.
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