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VOLUME 36 , NUMBER 1 PUBLISHED 15 DECEMBER 2020
SYNTHESIS PAPER
Dopamine Excess and/or Norepinephrine and Epinephrine Deficiency in Autistic Patients Due to Prenatal and/or Postnatal Deficiency of Dopamine Beta-Hydroxylase William Shaw Citation: Shaw W (2021) Dopamine excess and/or norepinephrine and epinephrine deficiency in autistic patients due to prenatal and/or postnatal deficiency of dopamine beta-hydroxylase. J Orthomol Med. 36(1) ABSTRACT
This review examines evidence of abnormal dopamine metabolism in autism over the last 40 years and examines environmental, microbial, and genetic factors that alter the activity of the enzyme dopamine-beta-hydroxylase which can account for the symptoms and biochemical abnormalities common in autism as well as the increased incidence of autism over the last 30 years. The marked increase in the worldwide application of the herbicide glyphosate to crops that have been genetically modified to be glyphosate tolerant is strongly correlated with the increased rate of autism. The use of this herbicide also alters the microbiome of the world, greatly diminishing beneficial microorganisms like Lactobacilli and Bifidobacteria, while increasing pathogenic bacteria species like Clostridia which have been found in increased amounts in autism. Clostridia species produce inhibitors of dopamine-beta-hydroxylase which cause excess dopamine and reduced norepinephrine which may lead to immune deficiency. These inhibitors produced by Clostridia have been confirmed as present in significantly higher concentrations in urine samples of people with autism. Mothers with deficiency of dopamine beta-hydroxylase in pregnancy have increased risk of having children with autism. Control of Clostridia bacteria and diminished use of glyphosate may offer a public health approach to diminish the incidence of autism. INTRODUCTION
Autism spectrum disorders are characterized by a behavioral syndrome that is recognized between ages 2 and 3 years. The core of the syndrome is a deviant and (or)
retarded development of cognitive capacities and skills necessary for social relations, communication, fantasy, and symbolic thinking. Almost all autistic people do not reach independence as adults, and 75% are mentally retarded as well (Shaw, Kassen, and Chaves, 1995). Despite the fact that autism is considered by many leading researchers to be one of the most genetic of all multifactorial neurodevelopmental disorders, with a concordance rate of over 50% between monozygotic (identical) twins versus less than 5% for dizygotic (fraternal) twins (Previc, 2007) and despite the fact that those with autism rarely marry and thereby pass on their genes, there has been a dramatic increase in autism in all industrialized nations (and especially the United States) over the past 25 years which is difficult to explain based solely based on genetic factors. Even in the case of the recently discovered ARHGEF6 gene single nucleotide polymorphism (SNP) on the X-chromosome, which accounts for about 30% of the cases of autism in males, 20% of those males with this gene SNP do not have autism (Pratt-Hyatt, Haeusler, Yuen, and Shaw, 2018). Abnormalities in the metabolism of dopamine in autism have been reported in the research literature for 40 years (Lelord et al (1978). Both Lelord et al (1978) and Garreau et al (1980) reported that urinary HVA levels were higher in autistic than in normal children. LeLord et al (1978) reported that the clinical improvement of these young autistic patients under vitamin B6 treatment was associated with a decrease of their urinary HVA excretion. Abnormalities in dopamine metabolism include elevated concentrations of the dopamine metabolite homovanillic acid (HVA) in cerebrospinal fluid (Cohen, Caparulo, Shaywitz, and Bower,
© 2021 International Society for Orthomolecular Medicine ISSN 0317-0209