pubmed.ncbi.nlm.nih.gov

Pharmacokinetics of L-carnitine - PubMed

Review

Pharmacokinetics of L-carnitine

Allan M Evans et al. Clin Pharmacokinet. 2003.

Abstract

L-Carnitine is a naturally occurring compound that facilitates the transport of fatty acids into mitochondria for beta-oxidation. Exogenous L-carnitine is used clinically for the treatment of carnitine deficiency disorders and a range of other conditions. In humans, the endogenous carnitine pool, which comprises free L-carnitine and a range of short-, medium- and long-chain esters, is maintained by absorption of L-carnitine from dietary sources, biosynthesis within the body and extensive renal tubular reabsorption from glomerular filtrate. In addition, carrier-mediated transport ensures high tissue-to-plasma concentration ratios in tissues that depend critically on fatty acid oxidation. The absorption of L-carnitine after oral administration occurs partly via carrier-mediated transport and partly by passive diffusion. After oral doses of 1-6g, the absolute bioavailability is 5-18%. In contrast, the bioavailability of dietary L-carnitine may be as high as 75%. Therefore, pharmacological or supplemental doses of L-carnitine are absorbed less efficiently than the relatively smaller amounts present within a normal diet.L-Carnitine and its short-chain esters do not bind to plasma proteins and, although blood cells contain L-carnitine, the rate of distribution between erythrocytes and plasma is extremely slow in whole blood. After intravenous administration, the initial distribution volume of L-carnitine is typically about 0.2-0.3 L/kg, which corresponds to extracellular fluid volume. There are at least three distinct pharmacokinetic compartments for L-carnitine, with the slowest equilibrating pool comprising skeletal and cardiac muscle.L-Carnitine is eliminated from the body mainly via urinary excretion. Under baseline conditions, the renal clearance of L-carnitine (1-3 mL/min) is substantially less than glomerular filtration rate (GFR), indicating extensive (98-99%) tubular reabsorption. The threshold concentration for tubular reabsorption (above which the fractional reabsorption begins to decline) is about 40-60 micromol/L, which is similar to the endogenous plasma L-carnitine level. Therefore, the renal clearance of L-carnitine increases after exogenous administration, approaching GFR after high intravenous doses. Patients with primary carnitine deficiency display alterations in the renal handling of L-carnitine and/or the transport of the compound into muscle tissue. Similarly, many forms of secondary carnitine deficiency, including some drug-induced disorders, arise from impaired renal tubular reabsorption. Patients with end-stage renal disease undergoing dialysis can develop a secondary carnitine deficiency due to the unrestricted loss of L-carnitine through the dialyser, and L-carnitine has been used for treatment of some patients during long-term haemodialysis. Recent studies have started to shed light on the pharmacokinetics of L-carnitine when used in haemodialysis patients.

PubMed Disclaimer

Cited by

The Anti-Adiposity Mechanisms of Ampelopsin and Vine Tea Extract in High Fat Diet and Alcohol-Induced Fatty Liver Mouse Models.
Wu J, Miyasaka K, Yamada W, Takeda S, Shimizu N, Shimoda H. Wu J, et al. Molecules. 2022 Jan 18;27(3):607. doi: 10.3390/molecules27030607. Molecules. 2022. PMID: 35163881 Free PMC article.
Enhanced bioavailability of L-carnitine after painless intradermal delivery vs. oral administration in rats.
Zhang S, Qin G, Wu Y, Gao Y, Qiu Y, Li F, Xu B. Zhang S, et al. Pharm Res. 2011 Jan;28(1):117-23. doi: 10.1007/s11095-010-0109-7. Epub 2010 Apr 13. Pharm Res. 2011. PMID: 20387100
Colon OCTN2 gene expression is up-regulated by peroxisome proliferator-activated receptor gamma in humans and mice and contributes to local and systemic carnitine homeostasis.
D'Argenio G, Petillo O, Margarucci S, Torpedine A, Calarco A, Koverech A, Boccia A, Paolella G, Peluso G. D'Argenio G, et al. J Biol Chem. 2010 Aug 27;285(35):27078-27087. doi: 10.1074/jbc.M110.109678. Epub 2010 Jun 17. J Biol Chem. 2010. PMID: 20558736 Free PMC article.
Carnitine transporter and holocarboxylase synthetase deficiencies in The Faroe Islands.
Lund AM, Joensen F, Hougaard DM, Jensen LK, Christensen E, Christensen M, Nørgaard-Petersen B, Schwartz M, Skovby F. Lund AM, et al. J Inherit Metab Dis. 2007 Jun;30(3):341-9. doi: 10.1007/s10545-007-0527-9. Epub 2007 Apr 6. J Inherit Metab Dis. 2007. PMID: 17417720
A randomised, controlled clinical trial evaluating changes in therapeutic efficacy and oxidative parameters after treatment with propionyl L-carnitine in patients with peripheral arterial disease requiring haemodialysis.
Signorelli SS, Fatuzzo P, Rapisarda F, Neri S, Ferrante M, Oliveri Conti G, Fallico R, Di Pino L, Pennisi G, Celotta G, Massimiliano A. Signorelli SS, et al. Drugs Aging. 2006;23(3):263-70. doi: 10.2165/00002512-200623030-00008. Drugs Aging. 2006. PMID: 16608381 Clinical Trial.

References

1. J Nutr. 1991 Apr;121(4):539-46 - PubMed
1. Anal Biochem. 1995 Oct 10;231(1):27-33 - PubMed
1. Gastroenterology. 1996 Dec;111(6):1534-40 - PubMed
1. Am J Physiol. 1985 Mar;248(3 Pt 1):G313-9 - PubMed
1. Anal Biochem. 1990 Feb 15;185(1):29-35 - PubMed

Pharmacokinetics of L-carnitine - PubMed