Controlled Clinical Trial of Dichloroacetate for Treatment of Congenital Lactic Acidosis in Children

Open-label studies indicate that oral dichloroacetate (DCA) may be effective in treating patients with congenital lactic acidosis. We tested this hypothesis by conducting the first double-blind, randomized, control trial of DCA in this disease. Forty-three patients who ranged in age from 0.9 to 19 y...

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Published in:Pediatrics (Evanston) 2006-05, Vol.117 (5), p.1519-1531
Main Authors: Stacpoole, Peter W, Kerr, Douglas S, Barnes, Carie, Bunch, S. Terri, Carney, Paul R, Fennell, Eileen M, Felitsyn, Natalia M, Gilmore, Robin L, Greer, Melvin, Henderson, George N, Hutson, Alan D, Neiberger, Richard E, O'Brien, Ralph G, Perkins, Leigh Ann, Quisling, Ronald G, Shroads, Albert L, Shuster, Jonathan J, Silverstein, Janet H, Theriaque, Douglas W, Valenstein, Edward
Format: Article
Language:English
Subjects:
Acidosis, Lactic - congenital
Acidosis, Lactic - drug therapy
Acidosis, Lactic - metabolism
Adolescent
Adult
Biological and medical sciences
Care and treatment
Child
Child, Preschool
Children
Children & youth
Clinical outcomes
Clinical trials
Congenital diseases
Dichloroacetic Acid - adverse effects
Dichloroacetic Acid - pharmacokinetics
Dichloroacetic Acid - therapeutic use
Drug therapy
Female
General aspects
Health aspects
Humans
Infant
Lactates - metabolism
Lactic acidosis
Male
Medical sciences
Metabolic disorders
Mitochondrial Diseases - drug therapy
Mitochondrial Diseases - metabolism
Neurologic Examination
Neuropsychological Tests
Pediatrics
Pyruvate Dehydrogenase Complex Deficiency Disease - drug therapy
Pyruvate Dehydrogenase Complex Deficiency Disease - metabolism
Quality of Life
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Summary:Open-label studies indicate that oral dichloroacetate (DCA) may be effective in treating patients with congenital lactic acidosis. We tested this hypothesis by conducting the first double-blind, randomized, control trial of DCA in this disease. Forty-three patients who ranged in age from 0.9 to 19 years were enrolled. All patients had persistent or intermittent hyperlactatemia, and most had severe psychomotor delay. Eleven patients had pyruvate dehydrogenase deficiency, 25 patients had 1 or more defects in enzymes of the respiratory chain, and 7 patients had a mutation in mitochondrial DNA. Patients were preconditioned on placebo for 6 months and then were randomly assigned to receive an additional 6 months of placebo or DCA, at a dose of 12.5 mg/kg every 12 hours. The primary outcome results were (1) a Global Assessment of Treatment Efficacy, which incorporated tests of neuromuscular and behavioral function and quality of life; (2) linear growth; (3) blood lactate concentration in the fasted state and after a carbohydrate meal; (4) frequency and severity of intercurrent illnesses and hospitalizations; and (5) safety, including tests of liver and peripheral nerve function. There were no significant differences in Global Assessment of Treatment Efficacy scores, linear growth, or the frequency or severity of intercurrent illnesses. DCA significantly decreased the rise in blood lactate caused by carbohydrate feeding. Chronic DCA administration was associated with a fall in plasma clearance of the drug and with a rise in the urinary excretion of the tyrosine catabolite maleylacetone and the heme precursor delta-aminolevulinate. In this highly heterogeneous population of children with congenital lactic acidosis, oral DCA for 6 months was well tolerated and blunted the postprandial increase in circulating lactate. However, it did not improve neurologic or other measures of clinical outcome.
ISSN:0031-4005
1098-4275
DOI:10.1542/peds.2005-1226