Nutritional and Metabolic Biomarkers in Autism Spectrum Disorders: An Exploratory Study

Anna E Esparham; Teri Smith; John M Belmont; Michael Haden; Leigh E Wagner; Randall G Evans; Jeanne A Drisko

Nutritional and Metabolic Biomarkers in Autism Spectrum Disorders: An Exploratory Study

Integr Med (Encinitas). 2015 Apr;14(2):40-53.

Authors

Anna E Esparham¹, Teri Smith², John M Belmont³, Michael Haden⁴, Leigh E Wagner¹, Randall G Evans¹, Jeanne A Drisko¹

Affiliations

¹ Integrative medicine department at the University of Kansas Medical Center (KUMC) in Kansas City, Kansas.
² Department of Psychiatry and Behavioral Sciences/Division of Psychology at KUMC.
³ Department of Pediatrics at KUMC.
⁴ School of Medicine-Wichita, University of Kansas.

PMID: 26770138
PMCID: PMC4566479

Abstract

Context: Autism spectrum disorder (ASD) is currently on the rise, now affecting approximately 1 in 68 children in the United States according to a 2010 surveillance summary from the Centers for Disease Control and Prevention (CDC). This figure is an estimated increase of 78% from the figure in 2002. The CDC suggests that more investigation is needed to understand this astounding increase in autism in such a short period.

Objective: The aim of this pilot study was to determine whether a group of children with ASD exhibited similar variations in a broad array of potential correlates, including medical histories, symptoms, genetics, and multiple nutritional and metabolic biomarkers.

Design: This study was a retrospective, descriptive chart review.

Setting: The study took place at the University of Kansas Medical Center (KUMC).

Participants: Participants were 7 children with ASD who had sought treatment at the Integrative Medicine Clinic at the medical center.

Results: A majority of the children exhibited an elevated copper:zinc ratio and abnormal vitamin D levels. Children also demonstrated abnormal levels of the essential fatty acids: (1) α-linolenic acid (ALA)- C13:3W3, and (2) linoleic acid (LA)-C18:2W6; high levels of docosahexaenoic acid (DHA); and an elevated ω-6:ω-3 ratio. Three of 7 children demonstrated abnormal manganese levels. Children did not demonstrate elevated urine pyruvate or lactate but did have abnormal detoxification markers. Three of 7 patients demonstrated abnormalities in citric acid metabolites, bacterial metabolism, and fatty acid oxidation markers. A majority demonstrated elevated serum immunoglobulin G (IgG) antibodies to casein, egg whites, egg yolks, and peanuts. A majority had absent glutathione S-transferase (GSTM) at the 1p13.3 location, and 3 of 7 children were heterozygous for the glutathione S-transferase I105V (GSTP1). A majority also exhibited genetic polymorphism of the mitochondrial gene superoxide dismutase A16V (SOD2).

Conclusions: The findings from this small group of children with ASD points to the existence of nutritional, metabolic, and genetic correlates of ASD. These factors appear to be important potential abnormalities that warrant a case control study to evaluate their reliability and validity as markers of ASD.