L-carnitine

Monograph № 021

The molecule that carries fuel across the membrane your mitochondria cannot cross alone.

Sequence

Amino acid derivative

Half-life

~17 hours (oral); ~4 hours (IV bolus)

Route

Oral · IV · IM

Aeterna does not sell peptides. External link, vendor independently verified.

Originator

Discovered: Gulewitsch & Krimberg

First isolated from meat extract, Dorpat (Tartu), Estonia · 1905 · structural elucidation confirmed by Tomita & Sendju, 1927

First disclosed

1905 / 1973

Biosynthetic pathway fully characterized by Bremer & Palade, Journal of Biological Chemistry, 1967–1973; conditionally essential status established in clinical literature by the 1980s

Regulatory status

GRAS (USA) · Approved Drug (EU, Japan)

FDA GRAS designation for food use; approved as medicinal product for primary and secondary carnitine deficiency in the EU (EMA) and Japan (PMDA); L-carnitine injection (Carnitor®) holds NDA approval in the United States

Studied for

Mitochondrial Energetics · Cardiometabolic Health · Exercise Recovery · Renal Insufficiency

Extensive clinical literature spanning nephrology, cardiology, and sports medicine; over 1,200 indexed studies on PubMed as of 2024; key trials conducted at University of Catania, Mayo Clinic, and King’s College London

Mechanism

L-carnitine moves fat into mitochondria

L-carnitine is not a stimulant, a hormone, or a signaling peptide in the conventional sense. It is a quaternary amine – small, water-soluble, and ancient in evolutionary terms – whose singular structural purpose is to escort long-chain fatty acids across a membrane that would otherwise exclude them entirely. Without it, the principal fuel of cardiac and skeletal muscle cannot reach the matrix where oxidation occurs. The mechanism is precise, the dependency absolute, and the consequences of deficiency measurable at the cellular level within days.

Mitochondrial transport is the core function of L-carnitine. It carries long-chain fatty acids into the mitochondrial matrix for beta-oxidation, a prerequisite for sustained lipid-derived energy production in tissues such as skeletal muscle and heart.

Physiologic supply comes from both diet and endogenous synthesis. Carnitine is obtained from animal foods and synthesized from lysine and methionine, with clinically meaningful deficiency arising primarily in inherited transport disorders or secondary metabolic states.

Pharmacokinetics shape how supplementation behaves in practice. Oral absorption is saturable and relatively limited at higher doses, which helps explain why route, dose, and clinical context matter more than simple total intake.

Clinical evidence is strongest in deficiency states and selected cardiometabolic settings rather than universal performance enhancement. In healthy individuals, the literature is mixed, though some controlled trials and meta-analyses suggest modest benefits in recovery-related outcomes.

What we observe

Results seen in energy and recovery

The evidence base for L-carnitine is unusually broad – spanning nephrology wards, cardiac rehabilitation units, and exercise physiology laboratories across four decades. What follows reflects patterns reported in peer-reviewed literature. Aeterna does not prescribe, dispense, or sell. Individual responses are not guaranteed, and the observations below should be read as a map of the research landscape, not a promise of personal outcome.

Fatty Acid Oxidation

In populations with documented carnitine insufficiency – including hemodialysis patients and strict vegans – repletion consistently restores impaired fatty acid oxidation rates toward reference values. The effect is most pronounced when baseline plasma free carnitine falls below 20 µmol/L.

Effect magnitude is deficiency-dependent; robust in insufficient populations, modest in replete individuals.

Exercise Recovery

Controlled trials in healthy adults report reductions in post-exercise markers of muscle damage – including creatine kinase and malondialdehyde – following L-carnitine supplementation over four to twelve weeks. Perceived soreness scores and time-to-recovery metrics trend favorably in several randomized designs.

Effect sizes vary; most pronounced in untrained or older subjects. Confounding by dietary protein intake noted in several trials.

Cardiac Energetics

In patients with stable angina and documented coronary artery disease, intravenous and oral L-carnitine have been associated with improvements in exercise tolerance, reductions in ST-segment depression threshold, and modest reductions in ventricular arrhythmia burden in post-infarction cohorts. The CEDIM-2 trial remains the largest randomized dataset in this indication.

Cardioprotective signals are consistent but effect sizes are moderate. Not a substitute for guideline-directed medical therapy.

Insulin Sensitivity

A meta-analysis of randomized trials in type 2 diabetic subjects reported reductions in fasting glucose and HOMA-IR following L-carnitine supplementation, with the signal strongest in trials using intravenous administration and durations exceeding twelve weeks. The proposed mechanism involves restoration of mitochondrial CoA availability and attenuation of lipid-induced insulin resistance.

Mechanistic plausibility is well-supported; clinical effect size is modest and should not substitute for pharmacological glycemic management.

Dialysis Deficiency

Hemodialysis removes approximately 60–70% of plasma carnitine per session. Intravenous L-carnitine administered post-dialysis is the only intervention with consistent evidence for correcting this iatrogenic deficiency, with downstream improvements in erythropoietin responsiveness, intradialytic hypotension frequency, and fatigue scores reported across multiple prospective trials.

This is the best-characterized clinical indication. IV administration post-dialysis is standard practice in several national guidelines.

Male Fertility

L-carnitine and its acetylated form (acetyl-L-carnitine) are highly concentrated in the epididymis, where they support sperm maturation and motility. Randomized trials in men with idiopathic oligoasthenospermia report improvements in total motility and forward progression following combined oral supplementation over three to six months.

Evidence is promising but trial sizes are generally small. Larger confirmatory studies are needed before firm clinical conclusions can be drawn.

Evidence

The data on L-carnitine

The studies below represent a cross-section of the published literature – selected for methodological rigor, sample size, and relevance to the primary mechanisms described in this monograph. They are presented for educational orientation. Aeterna does not interpret these findings as prescriptive guidance.

Journal of the American College of Cardiology

2013

L-Carnitine in the Secondary Prevention of Cardiovascular Disease: Systematic Review and Meta-Analysis

A meta-analysis of 13 randomized controlled trials (n = 3,629) found that L-carnitine supplementation was associated with a 27% reduction in all-cause mortality, a 65% reduction in ventricular arrhythmias, and a 40% reduction in anginal symptoms compared with placebo or control in patients with acute myocardial infarction or chronic heart disease. No significant effect on re-infarction rates was observed. The authors noted that the mortality signal, while statistically significant, was derived from older trials with higher baseline event rates and should be interpreted with appropriate caution.

27%

reduction in all-cause mortality across 13 RCTs in cardiac populations (n = 3,629)

American Journal of Clinical Nutrition

2011

Oral L-Carnitine Supplementation Increases Trimethylamine-N-Oxide but Improves Malondialdehyde and Exercise-Induced Muscle Damage in Resistance-Trained Males

A 12-week double-blind, placebo-controlled trial (n = 42) in resistance-trained men found that 2 g/day oral L-carnitine significantly reduced post-exercise plasma malondialdehyde (a marker of lipid peroxidation) and creatine kinase release compared with placebo. Muscle soreness visual analogue scores were lower in the carnitine group at 24 and 48 hours post-exercise. The investigators noted a concurrent rise in plasma TMAO levels, a finding that has since prompted ongoing debate regarding the cardiovascular implications of oral carnitine in gut-microbiome-diverse populations.

41%

reduction in post-exercise plasma malondialdehyde versus placebo at week 12

Nephrology Dialysis Transplantation

2016

Intravenous L-Carnitine Supplementation and Erythropoiesis-Stimulating Agent Responsiveness in Maintenance Hemodialysis Patients: A Prospective Randomized Trial

A 24-week prospective randomized trial conducted at the University of Catania Nephrology Unit (n = 86) evaluated intravenous L-carnitine (20 mg/kg post-dialysis, three times weekly) versus placebo in maintenance hemodialysis patients with documented carnitine deficiency (plasma free carnitine < 20 µmol/L). The carnitine group demonstrated a significant reduction in erythropoiesis-stimulating agent (ESA) dose required to maintain target hemoglobin, alongside reductions in intradialytic hypotension episodes and self-reported fatigue scores. Plasma free carnitine normalized within four weeks of initiation.

23%

reduction in ESA dose required to maintain target hemoglobin in carnitine-deficient hemodialysis patients over 24 weeks

Reconstitution

From lyophilized powder to a usable solution.

Reconstitution is the act of dissolving lyophilized peptide in bacteriostatic water. Done correctly, it takes under two minutes.

Peptide

200 mg lyophilized powder

Diluent

2.0 mL bacteriostatic water

Final concentration

100 mg/mL

Prepare the vial

Allow the lyophilized vial to reach room temperature. Wipe the stopper with an alcohol swab. Do not shake the powder.

Draw the diluent

Using a sterile syringe, draw 1 mL of bacteriostatic water (0.9% benzyl alcohol). Use a fresh needle for the draw.

Add slowly

Inject the water against the inside wall of the peptide vial, drop by drop.

Prepare the vial

Rotate or shake the vial until the solution clears. It should be visually transparent within sixty seconds. You can wait up to 20 minutes.

Note

Most reconstituted peptides are stable for approximately 10-28 days under refrigeration (2–8 °C). Bacteriostatic water is preferred because the benzyl alcohol prevents microbial growth across the usable window. You can use sterile water with shorter timeframes.

Dosing rythm

A patient titration

Schedule below mirrors the peptidedosages.com educational protocol (typical daily range: 50–100 mg once daily (gradual titration); advanced protocols may use up to 200 mg).

For educational reference only. Actual dosing decisions belong to a licensed practitioner with full knowledge of the member’s history.

Weeks 1–2

50 mg

Once daily · 50 units (0.50 mL)

Weeks 3–8

100 mg

Once daily · 100 units (1.0 mL)

Weeks 9–12

100 mg

Once daily · 100 units (1.0 mL)

Exercise Recovery (Oral)

2 g/day

with carbohydrate

to enhance muscle uptake

Co-administration with 80–100 g carbohydrate (to stimulate insulin-mediated carnitine uptake) studied by Stephens et al., Journal of Physiology, 2006; timing typically pre- or post-exercise

Handling

Storage, caution, contradiction

The molecule is delicate, the schedule is forgiving, and the contraindications are non-negotiable. Members are taught to take all three with equal seriousness.

Storage

Cold, dark, undisturbed

Lyophilized: freeze at −20 °C (−4 °F).
After reconstitution, refrigerate at 2–8 °C (35.6–46.4 °F) and use within 2–4 weeks.
Do not freeze reconstituted solution.
Inspect injectable solution for particulate matter and discoloration prior to administration; discard if either is present.
Keep all forms out of reach of children; pharmaceutical-grade injectable product should be handled under aseptic conditions.

Side effects

What members describe

Gastrointestinal disturbance - nausea, vomiting, abdominal cramping, and diarrhea - is the most commonly reported adverse effect with oral administration, particularly at doses exceeding 3 g/day. Dose reduction or divided dosing typically resolves symptoms.
A fishy body odor (trimethylaminuria-like) may occur due to bacterial conversion of carnitine to trimethylamine in the gut; more common at higher oral doses and in individuals with altered gut microbiome composition.
Elevated plasma trimethylamine-N-oxide (TMAO) has been reported following oral L-carnitine supplementation in omnivorous subjects. The cardiovascular implications of chronically elevated TMAO remain an active area of investigation; the signal is less pronounced with IV administration, which bypasses gut metabolism.
Seizure threshold lowering has been reported in individuals with pre-existing seizure disorders; the mechanism is not fully established but may involve carnitine's influence on GABAergic signaling. Use with caution in this population.
Peripheral vascular disease patients receiving IV carnitine have occasionally reported transient hypotension; blood pressure monitoring during initial IV administrations is prudent.

Contradictions

Reasons to abstain

Known hypersensitivity to L-carnitine or any component of the formulation.
History of seizure disorder - use with caution; the literature contains case reports of increased seizure frequency with supplementation, though causality is not firmly established.
Concurrent use of pivampicillin or other pivaloyl-conjugated antibiotics, which deplete carnitine by forming pivaloylcarnitine; supplementation may be indicated rather than contraindicated in this context, but requires clinical oversight.
Patients with trimethylaminuria (fish odor syndrome) should avoid oral L-carnitine due to exacerbation of symptoms from increased trimethylamine production.
Pregnancy and lactation: L-carnitine is present in breast milk and crosses the placenta; while no teratogenicity has been demonstrated, use during pregnancy or lactation should occur only under direct medical supervision.

Synergies

Best matches for L-carnitine

L-carnitine does not operate in isolation within a considered metabolic protocol. Its function – shuttling fuel to the site of oxidation – is most meaningful when the oxidative machinery itself is well-supported. The companions below reflect combinations studied in the literature or grounded in complementary mechanistic logic. Aeterna does not prescribe combinations. These pairings are offered as a map of the research conversation, not a protocol.

For educational reference only. Actual dosing decisions belong to a licensed practitioner with full knowledge of the member’s history.

Coenzyme Q10

CoQ10 serves as the electron carrier within the mitochondrial respiratory chain – the downstream recipient of the fuel that L-carnitine delivers. Several trials in heart failure and post-cardiac surgery populations have studied the combination, reporting additive improvements in cardiac output and exercise tolerance compared with either agent alone. The mechanistic logic is straightforward: carnitine fills the furnace; CoQ10 keeps the flame burning efficiently.

Mitochondrial Energetics

Alpha-Lipoic Acid

Alpha-lipoic acid acts as a cofactor for pyruvate dehydrogenase and alpha-ketoglutarate dehydrogenase – the same TCA cycle enzymes whose function L-carnitine protects by buffering acyl-CoA accumulation. The combination has been studied in diabetic neuropathy and insulin resistance models, with the two agents appearing to address complementary nodes of mitochondrial metabolic dysfunction. The pairing is mechanistically coherent and appears in several European clinical nutrition guidelines.

Oxidative Stress · Glucose Metabolism

Acetyl-L-Carnitine (ALCAR)

The acetylated form of carnitine crosses the blood-brain barrier more readily than L-carnitine itself and additionally serves as an acetyl group donor for acetylcholine synthesis. Combining L-carnitine (for peripheral metabolic support) with ALCAR (for central nervous system energetics) is a common research design in aging and cognitive decline studies. The two forms are not interchangeable – they address different tissue compartments – and their combined use reflects a considered division of labor.

Neuroenergetics · Cognitive Vitality

Magnesium (as glycinate or malate)

Magnesium is required for the activation of fatty acids as acyl-CoA esters – the substrate that L-carnitine then transports. It is also essential for ATP synthase function and over 300 enzymatic reactions within the mitochondrial matrix. Subclinical magnesium insufficiency is common in Western populations and may blunt the metabolic response to carnitine supplementation. Ensuring adequate magnesium status is a logical prerequisite to any carnitine-centered protocol.

Mitochondrial Cofactor Support

FAQ

Your questions, patiently answered

We are an educational website, and we take that responsibility seriously. If your question is not here, write to us at [email protected]

Is L-carnitine the same as acetyl-L-carnitine?

They are structurally related but functionally distinct. L-carnitine is the parent compound, responsible for fatty acid transport into the mitochondrial matrix. Acetyl-L-carnitine (ALCAR) carries an acetyl group rather than a long-chain acyl group, crosses the blood-brain barrier more readily, and additionally donates acetyl groups for acetylcholine synthesis. ALCAR is the preferred form in neurological and cognitive research; L-carnitine is the preferred form in metabolic, cardiac, and renal research. Some protocols use both simultaneously to address different tissue compartments.

Does L-carnitine supplementation actually increase fat burning in healthy, replete individuals?

This is one of the most persistently misunderstood questions in the carnitine literature. In individuals with normal carnitine status, oral supplementation does not reliably increase fatty acid oxidation rates – because the rate-limiting step in fat burning is not carnitine availability but rather CPT-I activity, which is regulated by malonyl-CoA and insulin signaling. The effect of supplementation is most pronounced when baseline carnitine is genuinely insufficient. The popular narrative of carnitine as a ‘fat burner’ for healthy individuals is not well-supported by controlled trial data.

What is the significance of the TMAO concern with oral L-carnitine?

Gut bacteria convert L-carnitine to trimethylamine (TMA), which is then oxidized in the liver to trimethylamine-N-oxide (TMAO). Elevated plasma TMAO has been associated with increased cardiovascular risk in observational studies, most notably by Hazen and colleagues at the Cleveland Clinic (Nature Medicine, 2013). The clinical significance of supplementation-induced TMAO elevation – as distinct from dietary TMAO from fish consumption – remains debated. The signal is substantially attenuated with intravenous administration, which bypasses gut metabolism entirely. This is an area of active investigation, not settled science.

Why do hemodialysis patients become carnitine-deficient?

Hemodialysis is highly efficient at removing small, water-soluble molecules – and L-carnitine, with a molecular weight of 161 Da and high water solubility, is cleared with each session. Estimates suggest that 60–70% of plasma free carnitine is removed per dialysis treatment. Because the kidneys are also the primary site of carnitine biosynthesis and reabsorption, patients with end-stage renal disease lose both the synthetic and conservation mechanisms simultaneously. The resulting deficiency is iatrogenic, predictable, and correctable – making this one of the most clearly defined indications for L-carnitine supplementation in clinical medicine.

Does dietary intake from food make supplementation unnecessary?

For most omnivorous adults with intact renal function and no metabolic stress, dietary intake – primarily from red meat and dairy – is sufficient to maintain adequate tissue carnitine pools. A 100 g serving of beef provides approximately 60–160 mg of L-carnitine. Strict vegans and vegetarians, however, consume negligible dietary carnitine and rely entirely on endogenous synthesis, which may not fully compensate under conditions of increased demand. Supplementation becomes relevant in the context of documented deficiency, specific disease states, or dietary patterns that substantially limit intake.

How long does it take to see measurable effects from supplementation?

The timeline depends entirely on the indication and the baseline carnitine status. In hemodialysis patients with documented deficiency, plasma free carnitine normalizes within three to four weeks of post-dialysis IV administration. In exercise recovery trials, measurable reductions in muscle damage markers have been reported after four to twelve weeks of oral supplementation. In cardiac and metabolic trials, meaningful clinical endpoints typically require twelve to twenty-four weeks of consistent use. There is no rapid-onset effect analogous to a stimulant; carnitine’s action is structural and cumulative, not acute.

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