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L-Carnitine

Related Terms

  • AcCn, acetyl-L-carnitine, B (t) Factor, β-hydroxy-gamma-N-trimethylamino butyrate, carnitene, carnitine, carnitor, canitor, D-carnitine, D,L-carnitine, LAC, L-acetyl-carnitine, LCLT, L-carnitina, L-carnitine L-tartrate, L-CARNIPURE, levacecarnine, levocarnitine, levocarnitine chloride, LK-80, L-propionylcarnitine, propionil-L-carnitine, propionyl-L-carnitine, ST261, VitaCarn®, vitamin B(t), vitamin Bt.

Background

  • The main function of L-carnitine is to transfer long-chain fatty acids in the form of their acyl-carnitine esters across the inner mitochondrial membrane before beta-oxidation. In humans, it is synthesized in the liver, kidney, and brain and actively transported to other areas of the body. For example, 98% of the total body L-carnitine is confined to the skeletal and cardiac muscle at concentrations approximately 70 times higher than in the blood serum.
  • Supplementation may be necessary in rare cases of primary carnitine deficiency, which may be caused by a defect in carnitine biosynthesis, a defect in carnitine active transport into tissue, or a defect in renal (kidney) conservation of carnitine. Known conditions of secondary deficiency of carnitine (insufficiency), in which L-carnitine is effective, include chronic stable angina and intermittent claudication characterized by distinct tissue hypoxia (low oxygen levels). Another condition that may benefit from carnitine supplementation is decreased sperm motility.
  • Although use in preterm infants suggests carnitine supplementation may aid in maintaining or increasing plasma carnitine levels and possibly weight gain, carnitine is not routinely added to preterm total parenteral nutrition (TPN). However, soy-based infant formulas are fortified with carnitine to levels found in breast milk.
  • In 1986, the U.S. Food and Drug Administration (FDA) approved L-carnitine for use in primary carnitine deficiency. D-carnitine or DL-carnitine may cause secondary L-carnitine deficiency and should not be used.

Evidence Table

    Disclaimer

    These uses have been tested in humans or animals. Safety and effectiveness have not always been proven. Some of these conditions are potentially serious, and should be evaluated by a qualified healthcare provider.

    A Nutritional deficiencies (primary and secondary carnitine deficiency in adults)

    Carnitine supplementation, both intravenous (injection) and oral (by mouth), is indicated for cases of primary and secondary carnitine deficiency. Use of L-carnitine in primary carnitine deficiency restores plasma carnitine levels to nearly normal levels. Muscle carnitine levels may rise only slightly; however muscle function can be normalized.

    B Angina (chronic stable)

    Evidence from clinical trials suggests that L-carnitine and L-propionyl-carnitine (propionyl-L-carnitine) are effective in reducing symptoms of angina. Carnitine may not offer further benefit when patients continue conventional therapies. Additional study is needed to confirm these findings.

    B Peripheral vascular disease

    Propionyl-L-carnitine and L-carnitine may treat peripheral vascular disease, especially in patients with severe limitations in peripheral circulation. The comparative effectiveness of propionyl-L-carnitine and other recognized treatments is unclear. More study is needed to make a firm recommendation.

    C ADHD

    Only one study has examined the effects of L-carnitine in boys with ADHD. Although results were promising, additional study is needed before a strong recommendation can be made.

    C AIDS

    Carnitine may be beneficial in AIDS treatment by increasing proliferation of mononuclear cells and increasing CD4 counts. Additional study is needed to make a firm recommendation.

    C Alcoholism

    L-carnitine or acetyl-L-carnitine may be of benefit to alcoholics. Additional study is needed to make a firm recommendation.

    C Alzheimer’s disease

    Early evidence suggests the effectiveness of L-carnitine and/or acetyl-L-carnitine for Alzheimer’s disease. However, the evidence is mixed.

    C Arrhythmia (abnormal heart rhythms)

    Although preliminary results are promising, there is insufficient available evidence to recommend for or against this use.

    C Cerebral ischemia (lack of adequate blood flow to the brain)

    There are a limited number of studies showing a positive effect of L-acetyl-carnitine on cerebral blood flow and metabolism of the brain in patients who have suffered from stroke. Additional study is required before a firm recommendation can be made.

    C Congestive heart failure

    Although preliminary results are promising, there is insufficient available evidence to recommend for or against the use of carnitine for congestive heart failure.

    C Dementia (elderly)

    Most of the studies related to dementia suffer from various weaknesses. Although preliminary evidence is promising, there is insufficient available evidence to recommend for or against this use.

    C Depression

    Although preliminary evidence is promising, there is insufficient available evidence to recommend for or against the use of carnitine in the treatment of depression.

    C Diabetes mellitus

    It has been suggested that L-carnitine under constant infusion is able to increase insulin sensitivity in patients with diabetes mellitus type II and enhance glucose oxidation. Carnitine may also decrease fasting blood glucose and Lp(a). Additional study is needed before a firm recommendation can be made.

    C Diabetic neuropathy

    Early evidence suggests that acetyl-L-carnitine may be beneficial for individuals with diabetic neuropathy. Additional study is needed before a firm recommendation can be made.

    C Dialysis (CAPD)

    L-carnitine taken by mouth has been used in patients receiving continuous ambulatory peritoneal dialysis (CAPD), but does not appear to lead to the resolution of hypertriglyceridemia. Additional study is needed before a firm recommendation can be made.

    C Dialysis (hemodialysis)

    Although preliminary evidence is promising, there is insufficient available evidence to recommend for or against to the use of carnitine for hemodialysis patients.

    C Diphtheria (throat disease)

    Early studies suggest that carnitine may be beneficial for patients with diphtheria, mainly in terms of myocardial (heart) damage. However, additional study is needed to confirm these findings.

    C Erectile dysfunction

    Preliminary studies suggest that propionyl-L-carnitine, with acetyl-L-carnitine or sildenafil may be beneficial for patients with erectile dysfunction. However, more rigorous trials should be performed in order to recommend carnitine for routine use in erectile dysfunction.

    C Exercise performance

    Overall, the data is mixed in terms of benefits of L-carnitine for exercise performance. Until confirmed, a strong recommendation for L-carnitine cannot be made for increased exercise endurance.

    C Fatigue

    There are several promising reports on the use of L-carnitine for fatigue. However, additional study is warranted in this area.

    C Fragile X syndrome

    There is insufficient evidence to support the use of carnitine in the treatment of hyperactive behavior of fragile -X children.

    C Hepatic encephalopathy (brain disease)

    Preliminary evidence suggests L-carnitine may be of benefit to individuals with hepatic encephalopathy, in terms of ammonia levels and psychometric functioning. Additional study is needed to make a firm recommendation.

    C Huntington’s chorea/disease

    One preliminary study showed that L-acetyl-carnitine possesses neither efficacy nor toxicity towards the patients with Huntington’s disease. Further trials are required before a firm recommendation can be made.

    C Hyperlipoproteinemia (high levels of lipoprotein and cholesterol in the blood)

    Although preliminary evidence is promising, there is insufficient available evidence to recommend for or against the use of carnitine for hyperlipoproteinemia.

    C Hyperthyroidism

    Although preliminary evidence is promising, there is insufficient available evidence to recommend for or against the use of carnitine for hyperthyroidism.

    C Infertility (asthenospermia)

    Early evidence shows a positive effect for carnitine and/or acetyl-L-carnitine in terms of increased sperm motility. However, additional study is needed before a firm conclusion can be made.

    C Lactic acidosis

    Although early evidence appears promising, currently there is insufficient evidence to recommend carnitine in the treatment of lactic acidosis.

    C Liver disease (cirrhosis)

    Although early evidence appears promising, currently there is insufficient evidence to recommend carnitine in the treatment of liver cirrhosis.

    C Memory

    There are a limited number of studies relevant to the use of carnitine for memory. Carnitine does not appear to have any effect on memory. Additional study is needed before a firm recommendation can be made.

    C Myocardial infarction (heart attack)

    Currently there is insufficient evidence to support the use of carnitine for myocardial infarction (heart attack). Additional study is needed in this area.

    C Nutritional deficiencies (adults)

    Currently there is insufficient evidence to support the use of carnitine in the total parenteral nutrition for adults. Additional study is needed in this area.

    C Nutritional deficiencies (fullterm infants)

    Despite a large number of studies, it is not clear what effect, if any, the addition of carnitine has on weight gain in full term infants. Additional study is needed.

    C Nutritional deficiencies (premature infants)

    Despite a large number of studies, it is not clear what effect, if any, the addition of carnitine has on weight gain in premature infants. Additional study is needed.

    C Obesity

    Early evidence shows that L-carnitine may have no effect on weight loss in obese patients. Further studies are needed before a firm recommendation can be made.

    C Peripheral neuropathy (nerve damage)

    Currently there is insufficient evidence to support the use of carnitine for peripheral neuropathy.

    C Peyronie’s disease

    Although early evidence is promising, more study is needed before a firm recommendation can be made.

    C Pregnancy (miscarriage)

    Currently there is insufficient evidence to support the use of carnitine for miscarriage.

    C Respiratory distress (adults)

    Currently there is insufficient evidence to support the use of carnitine for respiratory distress in adults.

    C Respiratory distress (infants)

    Currently there is insufficient evidence to support the use of carnitine for respiratory distress in infants.

    C Rett’s syndrome

    There are promising results on the use of carnitine for this condition. Before a strong recommendation can be made, additional well-designed trials are needed.

    C Sickle cell disease

    Preliminary evidence suggests the absence of any therapeutic effect of propionyl-L-carnitine for sickle cell disease. Additional studies are required before a firm recommendation can be made.

    C Surgerical uses (bypass)

    The results of studies on the use of carnitine in improving the functioning of myocardium (heart muscle) during open-heart surgery are controversial. Currently, there is insufficient available evidence to recommend for or against the use of carnitine.

    C Tuberculosis

    A preliminary study suggests antibacterial activity may be increased in patients with tuberculosis given acetyl-L-carnitine. Additional study is needed to confirm these findings.

*Key to grades:

Tradition

    Disclaimer

    The below uses are based on tradition, scientific theories, or limited research. They often have not been thoroughly tested in humans, and safety and effectiveness have not always been proven. Some of these conditions are potentially serious, and should be evaluated by a qualified healthcare provider. There may be other proposed uses that are not listed below.

Dosing

    Disclaimer

    The below doses are based on scientific research, publications, traditional use, or expert opinion. Many herbs and supplements have not been thoroughly tested, and safety and effectiveness may not be proven. Brands may be made differently, with variable ingredients, even within the same brand. The below doses may not apply to all products. You should read product labels, and discuss doses with a qualified healthcare provider before starting therapy.

  • Adults (18 years and older):

    • The U.S. Food and Drug Administration (FDA) recommends 1 gram of L-carnitine three times per day, intravenously (injected), for primary and secondary carnitine deficiency; this dose should not exceed 3 grams per day. A variety of doses have been used, with 3 grams per day in divided doses for 2-4 months being the most common; however, the doses range from 1 to 9 grams per day. Conditions treated have included AIDS, memory in alcoholics, Alzheimer’s disease, angina (chest pain), congestive heart failure, depression, diabetes, diabetic neuropathy, dialysis, exercise performance, hepatic encephalopathy, hyperlipdemia (high cholesterol), hyperthyroidism, myocardial infarction (heart attack), peripheral neuropathy (nerve damage), and peripheral vascular disease.
    • Intravenous injections have also been used, with doses typically ranging from 15-50 milligrams per kilogram twice daily. Injections have been given for seven days up to one year. Higher doses (up to 9 grams per day) have been studied. Injections should only be given under the supervision of a qualified healthcare professional, including a pharmacist.

  • Children (younger than 18 years):

    • The U.S. Food and Drug Administration (FDA) does not recommend exceeding 3 grams carnitine daily for primary and secondary carnitine deficiency. A typical dose for these deficiencies, as well as Rett’s syndrome, is 100-200 milligrams per kilogram taken daily divided over two or three doses. For hyperlipidemia (high cholesterol), 3 grams L-carnitine for up to six weeks has been used. For total parental nutrition in infants, 50 micromoles per kilogram for two weeks has been used. Injections should only be given under the supervision of a qualified healthcare professional, including a pharmacist,

Safety

    Disclaimer

    The U.S. Food and Drug Administration does not strictly regulate herbs and supplements. There is no guarantee of strength, purity or safety of products, and effects may vary. You should always read product labels. If you have a medical condition, or are taking other drugs, herbs, or supplements, you should speak with a qualified healthcare provider before starting a new therapy. Consult a healthcare provider immediately if you experience side effects.

  • Allergies

    • Avoid in individuals with a known allergy or hypersensitivity to carnitine.

  • Side Effects and Warnings

    • In general, L-carnitine is safe and no significant complications have been reported in available human clinical studies. Minor adverse effects have been reported with the use of L-carnitine or acetyl-L-carnitine, such as skin rash, body odor, “fishy smell,” diarrhea, gastric pyrosis (heartburn), nausea, gastralgia (stomachache), loose bowel movement, nonspecific abdominal discomfort, or vomiting. Euphoria, insomnia, nervousness mania, depression, and aggression have also been reported, but primarily in patients with pre-existing psychiatric conditions.
    • Transient hair loss was reported in 1% of cases. Less birth weight was regained in low birth weight infants treated with L-carnitine.
    • Carnitine supplements should be used cautiously in patients with peripheral vascular disease, hypertension (high blood pressure), alcohol-induced liver cirrhosis, low birth weight infants, diabetics, and patients on hemodialysis.

  • Pregnancy and Breastfeeding

    • L-carnitine is not recommended in pregnant or breastfeeding women due to a lack of available scientific evidence.

Interactions

    Disclaimer

    Most herbs and supplements have not been thoroughly tested for interactions with other herbs, supplements, drugs, or foods. The interactions listed below are based on reports in scientific publications, laboratory experiments, or traditional use. You should always read product labels. If you have a medical condition, or are taking other drugs, herbs, or supplements, you should speak with a qualified healthcare provider before starting a new therapy.

  • Interactions with Drugs

    • Several drugs may affect the levels of carnitine in the body. For example, adefovir dipivoxil (Hepsera®), which is given for hepatitis B, may reduce free carnitine levels. Cephalosporin antibiotics may reduce plasma carnitine levels. Anticonvulsants (phenobarbital, phenytoin, carbamazepine) may decrease serum carnitine in children. Cisplastin may increase urinary excretion of carnitine. Ifosfamide (Mitoxana®), a chemotherapy drug, may increase urinary loss of carnitine; however, use of carnitine plus ifosfamide may help reduce fatigue (side effect of ifosfamide treatment). Patients suffering from neuropathy (nerve damage) induced by nucleosides may have reduced levels of acetyl carnitine. Penicillin derivatives (pivaloyloxymethyl esterified; pivampicillin and pivmecillinam) may decrease in serum carnitine concentration, elevate excretion of acyl-carnitine, and reduce muscle carnitine concentration in adults and children.
    • L-carnitine may decrease the need for certain drugs, such as glycosides, digoxin, diuretics, beta-blockers, channel blockers, hypolipidemic (cholesterol-altering) drugs, and nitro derivatives.
    • L-carnitine supplementation may reduce side effects associated with interleukin-2 (IL-2) or nortriptyline (Pamelor®, Aventyl®). It may also improve liver and muscular side effects associated with isotretinoin (Accutane®) in acne patients. Carnitine may reduce nerve damage symptoms associated with paclitaxel (Taxol®) use.
    • Carnitine may prevent arrhythmias (abnormal heart rhythms) provoked by adriamycin (Doxorubicin®), which is used in chemotherapy. L-carnitine may decrease the need for antiarrhythmics (medications used to treat abnormal rhythms in the heart). Carnitine plus propafenone may improve arrhythmia (heart rhythm) better than propafenone alone.
    • L-carnitine may decrease the need for anticoagulants (“blood thinners”), such as warfarin (Coumadin®) or heparin.
    • Several combinations have shown positive interactions. For example, sildenafil and propionyl-L-carnitine may be more effective than sildenafil alone. Although not well studied in humans, L-carnitine used concurrently with antiviral agents such as zidovudin(Retrovir®), or carnitine used with nortryptiline, may also have a positive interaction that reduces side effects. L-carnitine plus acetyl-L-carnitine plus cinnoxicam has been found more effective in improving sperm parameters as compared with L-carnitine plus acetyl-L-carnitine alone.
    • Patients with diabetes should use caution because L-carnitine may decrease blood sugar. However, carnitine levels did not change in diabetics using insulin or sulfonylurea therapy. It is unclear whether L-carnitine would have similar effects when combined with other medications that lower blood sugar. Consult with a qualified healthcare professional, including a pharmacist, before combining therapies.
    • Although not well studied in humans, carnitine may increase valproic acid concentrations in the brain, which might increase the effects of valproic acid. Caution is advised.

  • Interactions with Herbs and Dietary Supplements

    • L-carnitine may decrease the need for herbs or supplements with anticoagulant effects (“blood thinners”). L-carnitine may also decrease the need for herbs or supplements with diuretic effects. Dosing adjustments may be necessary.
    • Patients with diabetes should use caution because L-carnitine may decrease blood sugar. However, carnitine levels did not change in diabetics using insulin or sulfonylurea therapy. It is unclear whether L-carnitine would have similar effects when combined with other herbs and supplements that lower blood sugar. Consult with a qualified healthcare professional, including a pharmacist, before combining therapies.
    • Choline supplementation may reduce excretion, renal (kidney) clearance, and fractional clearance of non-esterified carnitine.
    • Rhabdomyolysis (a serious condition involving breakdown of skeletal muscle), a side effect of taking licorice by mouth, may be minimized with L-carnitine chloride and potassium chloride.

Attribution

  • This information is based on a systematic review of scientific literature edited and peer-reviewed by contributors to the Natural Standard Research Collaboration ().

Bibliography

    Disclaimer

    Natural Standard developed the above evidence-based information based on a thorough systematic review of the available scientific articles. For comprehensive information about alternative and complementary therapies on the professional level, go to . Selected references are listed below.

  • Bazzato G, Coli U, Landini S, et al. Myasthenia-like syndrome after D,L- but not L-carnitine. Lancet 5-30-1981;1(8231):1209.
    View Abstract
  • Bazzato G, Mezzina C, Ciman M, et al. Myasthenia-like syndrome associated with carnitine in patients on long- term haemodialysis. Lancet 5-12-1979;1(8124):1041-1042.
    View Abstract
  • Benvenga S, Ruggeri RM, Russo A, et al. Usefulness of L-carnitine, a naturally occurring peripheral antagonist of thyroid hormone action, in iatrogenic hyperthyroidism: a randomized, double-blind, placebo-controlled clinical trial. J Clin Endocrinol Metab 2001;86(8):3579-3594.
    View Abstract
  • Bohmer T, Bergrem H, Eiklid K. Carnitine deficiency induced during intermittent haemodialysis for renal failure. Lancet 1-21-1978;1(8056):126-128.
    View Abstract
  • Casciani CU, Caruso U, Cravotto E, et al. Effect of L-carnitine on lipid pattern in haemodialysis. Lancet 12-13-1980;2(8207):1309-1310.
    View Abstract
  • El Beshlawy A, Abd El Raouf, Mostafa F, et al. Diastolic dysfunction and pulmonary hypertension in sickle cell anemia: is there a role for L-carnitine treatment? Acta Haematol. 2006;115(1-2):91-96.
    View Abstract
  • Ellaway C, Williams K, Leonard H, et al. Rett syndrome: randomized controlled trial of L-carnitine. J Child Neurol 1999;14(3):162-167.
    View Abstract
  • Holme E, Greter J, Jacobson CE, et al. Carnitine deficiency induced by pivampicillin and pivmecillinam therapy. Lancet 8-26-1989;2(8661):469-473.
    View Abstract
  • Jirillo E, Altamura M, Munno I, et al. Effects of acetyl-L-carnitine oral administration on lymphocyte antibacterial activity and TNF-alpha levels in patients with active pulmonary tuberculosis. A randomized double blind versus placebo study. Immunopharmacol.Immunotoxicol. 1991;13(1-2):135-146.
    View Abstract
  • Lacour B, Di Giulio S, Chanard J, et al. Carnitine improves lipid anomalies in haemodialysis patients. Lancet 10-11-1980;2(8198):763-764.
    View Abstract
  • Maebashi M, Kawamura N, Sato M, et al. Lipid-lowering effect of carnitine in patients with type-IV hyperlipoproteinaemia. Lancet 10-14-1978;2(8094):805-807.
    View Abstract
  • Persico G, Amato B, Aprea G, et al. The early effects of intravenous L-propionyl carnitine on ulcerative trophic lesions of the lower limbs in arteriopathic patients: a controlled randomized study. Drugs Exp Clin Res 1995;21(5):187-198.
    View Abstract
  • Sima AA, Calvani M, Mehra M, et al. Acetyl-L-carnitine improves pain, nerve regeneration, and vibratory perception in patients with chronic diabetic neuropathy: an analysis of two randomized placebo-controlled trials. Diabetes Care 2005;28(1):89-94.
    View Abstract
  • Singh RB, Niaz MA, Agarwal P, et al. A randomised, double-blind, placebo-controlled trial of L-carnitine in suspected acute myocardial infarction. Postgrad.Med J 1996;72(843):45-50.
    View Abstract
  • Thomas S, Fischer FP, Mettang T, et al. Effects of L-carnitine on leukocyte function and viability in hemodialysis patients: A double-blind randomized trial. Am J Kidney Dis 1999;34(4):678-687.
    View Abstract