Acetylcarnitine Explained

Acetyl-L-carnitine, ALCAR or ALC, is an acetylated form of L-carnitine. It is naturally produced by the human body, and it is available as a dietary supplement. Acetylcarnitine is broken down in the blood by plasma esterases to carnitine which is used by the body to transport fatty acids into the mitochondria for breakdown and energy production.

Biochemical production and action

Carnitine is both a nutrient and made by the body as needed; it serves as a substrate for important reactions in which it accepts and gives up an acyl group. Acetylcarnitine is the most abundant naturally occurring derivative and is formed in the reaction:

acetyl-CoA + carnitine CoA + acetylcarnitine

where the acetyl group displaces the hydrogen atom in the central hydroxyl group of carnitine.[1] [2] Coenzyme A (CoA) plays a key role in the Krebs cycle in mitochondria, which is essential for the production of ATP, which powers many reactions in cells; acetyl-CoA is the primary substrate for the Krebs cycle, once it is de-acetylated, it must be re-charged with an acetyl-group in order for the Krebs cycle to keep working.[2]

Most cell types appear to have transporters to import carnitine and export acyl-carnitines, which seems to be a mechanism to dispose of longer-chain moieties; however many cell types can also import ALCAR.[1]

Within cells, carnitine plays a key role in importing acyl-CoA into mitochondria; the acyl-group of the acyl-CoA is transferred to carnitine, and the acyl-carnitine is imported through both mitochondrial membranes before being transferred to a CoA molecule, which is then beta oxidized to acetyl-CoA. A separate set of enzymes and transporters also plays a buffering role by eliminating acetyl-CoA from inside mitochondria created by the pyruvate dehydrogenase complex that is in excess of its utilization by the Krebs cycle; carnitine accepts the acetyl moiety and becomes ALCAR, which is then transported out of the mitochondria and into the cytosol, leaving free CoA inside the mitochondria ready to accept new import of fatty acid chains.[2] ALCAR in the cytosol can also form a pool of acetyl-groups for CoA, should the cell need it.[2]

Excess acetyl-CoA causes more carbohydrates to be used for energy at the expense of fatty acids. This occurs by different mechanisms inside and outside the mitochondria. ALCAR transport decreases acetyl-CoA inside the mitochondria, but increases it outside.[3] [4]

Health effects

Carnitine and ALCAR supplements carry warnings of a risk that they promote seizures in people with epilepsy, but a 2016 review found this risk to be based only on animal trials.[5]

Research

Reviews

Meta-analyses from 2015 and 2017 both conclude that the current evidence suggests ALC reduces pain from peripheral neuropathy with few adverse effects.[6] The 2017 review also suggested ALC improved electromyographic parameters.[7] Both called for more randomized controlled trials. An updated Cochrane review in 2019 of four studies with 907 participants was very uncertain as to if ALC caused a pain reduction after 6 to 12 months of treatment.[8]

A 2015 Cochrane review of ALCAR in fragile X syndrome found only two placebo-controlled trials, each of low quality, and concluded that ALCAR is unlikely to improve intellectual functioning or hyperactive behavior in children with this condition.[17]

ALCAR has been studied in hepatic encephalopathy, a complication of cirrhosis involving neuropsychiatric impairment; ALCAR improves blood ammonia levels and generates a modest improvement in psychometric scores but does not resolve the condition – it may play a minor role in managing the condition.[18]

Studies

Other reviews

Notes and References

  1. Bieber LL . Carnitine . Annual Review of Biochemistry . 57 . 261–283 . 1988 . 3052273 . 10.1146/annurev.bi.57.070188.001401 .
  2. Stephens FB, Constantin-Teodosiu D, Greenhaff PL . New insights concerning the role of carnitine in the regulation of fuel metabolism in skeletal muscle . The Journal of Physiology . 581 . Pt 2 . 431–444 . June 2007 . 17331998 . 2075186 . 10.1113/jphysiol.2006.125799 .
  3. Kiens B . Skeletal muscle lipid metabolism in exercise and insulin resistance . Physiological Reviews . 86 . 1 . 205–243 . January 2006 . 16371598 . 10.1152/physrev.00023.2004 .
  4. Lopaschuk GD, Gamble J . The 1993 Merck Frosst Award. Acetyl-CoA carboxylase: an important regulator of fatty acid oxidation in the heart . Canadian Journal of Physiology and Pharmacology . 72 . 10 . 1101–1109 . October 1994 . 7882173 . 10.1139/y94-156 .
  5. Zeiler FA, Sader N, Gillman LM, West M . Levocarnitine induced seizures in patients on valproic acid: A negative systematic review . Seizure . 36 . 36–39 . March 2016 . 26889779 . 10.1016/j.seizure.2016.01.020 . free .
  6. Li S, Li Q, Li Y, Li L, Tian H, Sun X . Acetyl-L-carnitine in the treatment of peripheral neuropathic pain: a systematic review and meta-analysis of randomized controlled trials . PLOS ONE . 10 . 3 . e0119479 . 2015-01-01 . 25751285 . 4353712 . 10.1371/journal.pone.0119479 . free . 2015PLoSO..1019479L .
  7. Veronese N . 2017. Effect of acetyl-l-carnitine in the treatment of diabetic peripheral neuropathy: A systematic review and meta-analysis. European Geriatric Medicine. 8. 2. 117–122. 10.1016/j.eurger.2017.01.002. 10138/235591. 56342481 . free.
  8. Rolim LC, da Silva EM, Flumignan RL, Abreu MM, Dib SA . Acetyl-L-carnitine for the treatment of diabetic peripheral neuropathy . The Cochrane Database of Systematic Reviews . 2019 . 6 . CD011265 . June 2019 . 31201734 . 6953387 . 10.1002/14651858.CD011265.pub2 .
  9. Schloss JM, Colosimo M, Airey C, Masci PP, Linnane AW, Vitetta L . Nutraceuticals and chemotherapy induced peripheral neuropathy (CIPN): a systematic review . Clinical Nutrition . 32 . 6 . 888–893 . December 2013 . 23647723 . 10.1016/j.clnu.2013.04.007 .
  10. Brami C, Bao T, Deng G . Natural products and complementary therapies for chemotherapy-induced peripheral neuropathy: A systematic review . Critical Reviews in Oncology/Hematology . 98 . 325–334 . February 2016 . 26652982 . 4727999 . 10.1016/j.critrevonc.2015.11.014 .
  11. Ahmadi S, Bashiri R, Ghadiri-Anari A, Nadjarzadeh A . Antioxidant supplements and semen parameters: An evidence based review . International Journal of Reproductive Biomedicine . 14 . 12 . 729–736 . December 2016 . 28066832 . 5203687 . 10.29252/ijrm.14.12.729 .
  12. Arcaniolo D, Favilla V, Tiscione D, Pisano F, Bozzini G, Creta M, Gentile G, Menchini Fabris F, Pavan N, Veneziano IA, Cai T . 6 . Is there a place for nutritional supplements in the treatment of idiopathic male infertility? . Archivio Italiano di Urologia, Andrologia . 86 . 3 . 164–170 . September 2014 . 25308577 . 10.4081/aiua.2014.3.164 . free .
  13. Hudson S, Tabet N . Acetyl-L-carnitine for dementia . The Cochrane Database of Systematic Reviews . 2003 . 2 . CD003158 . 2003 . 12804452 . 6991156 . 10.1002/14651858.CD003158 . Systematic review .
  14. Wang SM, Han C, Lee SJ, Patkar AA, Masand PS, Pae CU . A review of current evidence for acetyl-l-carnitine in the treatment of depression . Journal of Psychiatric Research . 53 . 30–37 . June 2014 . 24607292 . 10.1016/j.jpsychires.2014.02.005 .
  15. Kriston L, von Wolff A, Westphal A, Hölzel LP, Härter M . Efficacy and acceptability of acute treatments for persistent depressive disorder: a network meta-analysis . Depression and Anxiety . 31 . 8 . 621–630 . August 2014 . 24448972 . 10.1002/da.22236 . 41163109 . free .
  16. Veronese N, Stubbs B, Solmi M, Ajnakina O, Carvalho AF, Maggi S . Acetyl-L-Carnitine Supplementation and the Treatment of Depressive Symptoms: A Systematic Review and Meta-Analysis . Psychosomatic Medicine . 80 . 2 . 154–159 . Feb–Mar 2018 . 29076953 . 10.1097/PSY.0000000000000537 . 7649619 .
  17. Rueda JR, Guillén V, Ballesteros J, Tejada MI, Solà I . L-acetylcarnitine for treating fragile X syndrome . The Cochrane Database of Systematic Reviews . 19 . 5 . CD010012 . May 2015 . 25985235 . 10.1002/14651858.CD010012.pub2 . 10849109 .
  18. Jawaro T, Yang A, Dixit D, Bridgeman MB . Management of Hepatic Encephalopathy: A Primer . The Annals of Pharmacotherapy . 50 . 7 . 569–577 . July 2016 . 27126547 . 1503997 . 10.1177/1060028016645826 . 32765158 .
  19. Liu J, Head E, Gharib AM, Yuan W, Ingersoll RT, Hagen TM, Cotman CW, Ames BN . 6 . Memory loss in old rats is associated with brain mitochondrial decay and RNA/DNA oxidation: Partial reversal by feeding acetyl-L-carnitine and/or R -α-lipoic acid . Proceedings of the National Academy of Sciences of the United States of America . 99 . 4 . 2356–2361 . February 2002 . 11854529 . 122369 . 10.1073/pnas.261709299 . free .