Guest guest Posted February 27, 2003 Report Share Posted February 27, 2003 Terri, Welcome to the list. There are quite a few parents on the list who have children with autism spectrum disorders. Have you seen the abstract from Dr. Kelley's talk to the Mitochondrial Interest Group Minisymposium in 2000? Here is the website: http://tango01.cit.nih.gov/sig/mito/webversion.pdf Abnormalities of Mitochondrial Metabolism in Children with Austistic Spectrum Disorders Although developmental delay is a common characteristic of children with disorders of mitochondrial metabolism, classical autism, Asperger syndrome, and PDD have not common been associated with mitochondrial disease. Because our institutions servers a large number of children with developmental disabilities, we have and the opportunity to diagnose many metabolic diseases among children with autistic spectrum disorders including including defects of organic acid, sterol, and mitochondrial metabolism. Among these, mitochondrial disease is the most common diagnostic category and represents a clinically significant fraction of autistic children. Although we find a variety of autistic phenotypes to have associated mitochondrial abnormalities, the most common is nonspecific PDD, typically of a form that language and cognitive regression or stagnation during the second year. Most surprising among multiplex families is that the biochemical and clinical markers of mitochondrial disease often segregate in an autosomal dominant dominant manner. Although no molecular lesion has yet been found in the autosomal dominant families, the biochemical findings are most consistent with abnormal complex I activity. Moreover, when identified below the age of two years, affected children often respond to therapy designed to augment complex I activity. We propose that, like the basal ganglia, areas of the brain important in language development and personal social interaction are especially vulnerable in the first two years to injury mediated by defects of mitochondrial energy metabolism, and that early and careful evaluation of autistic children from these more subtle mitochondrial disturbances may rescue them from more severe brain injury. Were you given any recommendations to augment Complex I activity? Quote Link to comment Share on other sites More sharing options...
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