Double-blind, placebo-controlled
Study of L- carnosine supplementation in children with autistic spectrum disorder
Michael G. Chez, M.D., Cathleen P. Buchanan, Ph.D., Jamie L. Komen, M.A.,
Marina Becker, R.N. Journal of Child Neurology (accepted for publication 2003).
Pediatric Neurology, Lake Forest Hospital, Illinois 60045, USA. mchezmd@interaccess.com
(PubMed
- Abstract)
Objective:
L-Carnosine
is an amino acid dipeptide that may enhance frontal lobe function. We therefore
sought to investigate whether L-Carnosine supplementation for children with Autistic
Spectrum Disorders (ASD) results in observable, objective changes in language
and/or behavior in contrast to placebo.
Design/Methods:
Thirty-one
children (21 M, mean age= 7.45; range = 3.2-12.5 yrs) meeting inclusion criteria
were enrolled in an 8 week blinded trial of either 400 mg BID powdered
L-Carnosine or placebo. Children were assessed at a pediatric neurology clinic
with the Childhood Autism Rating Scale (CARS), the Gilliam Autism Rating Scale
(GARS), the Expressive and Receptive One-Word Picture Vocabulary tests (E/ROWPVT),
and biweekly parental Clinical Global Impression of Change (CGI), at baseline
and 8 week endpoint.
Dr
Michael G. Chez
is specialist and associate professor in Child
Neurology
Results:
Children
who were on placebo (n=17) did not show statistically significant changes on any
of the outcome measures. After 8 weeks on L-Carnosine, children (n=14) showed
statistically significant improvements on the GARS total score, GARS Behavior,
Socialization, and Communication subscales, and the ROWPVT (all ps<.05).
E/ROWPVT and CARS showed trends in improvements, which were supported by parental
CGI.
Conclusions:
Oral supplementation with 400mg L-Carnosine
resulted in demonstrable improvements in autistic behaviors as well as increases
in language comprehension that reached statistical significance. Although
the mechanism of action of the amino acid is not well understood, it is believed
that it acts to modulate neurotransmission and affect metal ion transfer of zinc
and copper in the entorhinal cortex. This may enhance neurological function or
act in a neuroprotective fashion.
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