a secondary carnitine deficiency.

with caution and only where clinical and biochemical considerations make it seem likely that higher doses will be of benefit. dosage should start at 1 g/day, (10 ml/day), and be increased slowly while assessing tolerance and therapeutic response. monitoring should include periodic blood chemistries, vital signs, plasma carnitine concentrations, and overall clinical condition. infants and children: the recommended dosage of levocarnitine is 50 to 100 mg/kg/day which is equivalent to 0.5 ml/kg/day carnitor ® (levocarnitine) oral solution or carnitor ® sf (levocarnitine) sugar-free oral solution. higher doses should be administered only with caution and only where clinical and biochemical considerations make it seem likely that higher doses will be of benefit. dosage should start at 50 mg/kg/day, and be increased slowly to a maximum of 3 g/day (30 ml/day) while assessing tolerance and therapeutic response. monitoring should include periodic blood chemistries, vital signs, plasma carnitine concentrations, and overall clinical condition. carnitor ® (levocarnitine) oral solution or carnitor ® sf (levocarnitine) sugar-free oral solution may be consumed alone or dissolved in drink or other liquid food. doses should be spaced evenly throughout the day (every three or four hours) preferably during or following meals and should be consumed slowly in order to maximize tolerance.

hould be monitored very closely during the first week of administration, and after any dosage increases. musculoskeletal reactions : mild myasthenia has been described only in uremic patients receiving d,l-carnitine. neurologic reactions : seizures have been reported to occur in patients with or without pre-existing seizure activity receiving either oral or intravenous levocarnitine. in patients with pre-existing seizure activity, an increase in seizure frequency and/or severity has been reported. hypersensitivity reactions : rash, urticaria, and facial edema have been reported with oral carnitor ® (see warnings ).

ioaccumulate acylcoa esters. 1-6 secondary carnitine deficiency can be a consequence of inborn errors of metabolism. carnitor ® may alleviate the metabolic abnormalities of patients with inborn errors that result in accumulation of toxic organic acids. conditions for which this effect has been demonstrated are: glutaric aciduria ii, methyl malonic aciduria, propionic acidemia, and medium chain fatty acylcoa dehydrogenase deficiency. 7,8 autointoxication occurs in these patients due to the accumulation of acylcoa compounds that disrupt intermediary metabolism. the subsequent hydrolysis of the acylcoa compound to its free acid results in acidosis which can be life-threatening. levocarnitine clears the acylcoa compound by formation of acylcarnitine, which is quickly excreted. carnitine deficiency is defined biochemically as abnormally low plasma concentrations of free carnitine, less than 20 µmol/l at one week post term and may be associated with low tissue and/or urine concentrations. further, this condition may be associated with a plasma concentration ratio of acylcarnitine/levocarnitine greater than 0.4 or abnormally elevated concentrations of acylcarnitine in the urine. in premature infants and newborns, secondary deficiency is defined as plasma levocarnitine concentrations below age-related normal concentrations.

tions of carnitor ® , calculated after correction for circulating endogenous plasma concentrations of levocarnitine, was 15.1 ± 5.3% for carnitor ® tablets and 15.9 ± 4.9% for carnitor ® oral solution. total body clearance of levocarnitine (dose/auc including endogenous baseline concentrations) was a mean of 4.00 l/h. levocarnitine was not bound to plasma protein or albumin when tested at any concentration or with any species including the human. 9