International Meeting for Autism Research: Nutritional and Metabolic Status of Children with Autism

Nutritional and Metabolic Status of Children with Autism

Friday, May 13, 2011
Elizabeth Ballroom E-F and Lirenta Foyer Level 2 (Manchester Grand Hyatt)
2:00 PM
J. Adams
Background:  

There is growing evidence of multiple metabolic problems in children with autism, including oxidative stress, methylation problems, sulfation deficits, and nutritional insufficiencies.

Objectives:  

1)  Compare the nutritional and metabolic status of children with autism with that of neurotypical children 

2)  Investigates the possible association of autism severity with biomarkers of nutritional and metabolic status.

Methods:  

Participants were children ages 5-16 years in Arizona with Autistic Spectrum Disorder (n=55) compared with non-sibling, neurotypical controls (n=44) of similar age, gender and geographical distribution.  Neither group had taken any vitamin/mineral supplements in the two months prior to sample collection.  Autism severity was assessed using the Pervasive Development Disorder Behavior Inventory (PDD-BI), Autism Treatment Evaluation Checklist (ATEC), and Severity of Autism Scale (SAS). Study measurements included: vitamins, biomarkers of vitamin status, minerals, plasma amino acids, plasma glutathione, and biomarkers of oxidative stress, methylation, sulfation and energy production.

Results:  

Biomarkers of children with autism compared to those of controls using a t-test or Wilcoxon test found the following statistically significant differences (p<0.001):   Low levels of biotin, plasma glutathione, RBC SAM, plasma uridine, plasma ATP, RBC NADH, RBC NADPH, plasma sulfate (free and total), and plasma tryptophan; also high levels of oxidative stress markers and plasma glutamate. Levels of biomarkers for the neurotypical controls were in good agreement with accessed published reference ranges.  In the Autism group, mean levels of vitamins, minerals, and most amino acids commonly measured in clinical care were within published reference ranges.   

A stepwise, multiple linear regression analysis demonstrated significant associations between several groups of biomarkers with all three autism severity scales, including vitamins (adjusted R2 of 0.25-0.57), minerals (adj. R2 of 0.22-0.38), and plasma amino acids (adj. R2 of 0.22-0.39). 

Conclusions:  

The autism group had many statistically significant differences in their nutritional and metabolic status, including biomarkers indicative of vitamin insufficiency, increased oxidative stress, reduced capacity for energy transport, sulfation and detoxification.  Several of the biomarker groups were significantly associated with variations in the severity of autism.  These nutritional and metabolic differences are generally in agreement with other published results and are likely amenable to nutritional supplementation.  Research investigating treatment and its relationship to the co-morbidities and etiology of autism is warranted.

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