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      Clinical and Molecular Characteristics of Mitochondrial Dysfunction in Autism Spectrum Disorder

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          Abstract

          Autism spectrum disorder (ASD) affects ~ 2% of children in the United States. The etiology of ASD likely involves environmental factors triggering physiological abnormalities in genetically sensitive individuals. One of these major physiological abnormalities is mitochondrial dysfunction, which may affect a significant subset of children with ASD. Here we systematically review the literature on human studies of mitochondrial dysfunction related to ASD. Clinical aspects of mitochondrial dysfunction in ASD include unusual neurodevelopmental regression, especially if triggered by an inflammatory event, gastrointestinal symptoms, seizures, motor delays, fatigue and lethargy. Traditional biomarkers of mitochondrial disease are widely reported to be abnormal in ASD, but appear non-specific. Newer biomarkers include buccal cell enzymology, biomarkers of fatty acid metabolism, non-mitochondrial enzyme function, apoptosis markers and mitochondrial antibodies. Many genetic abnormalities are associated with mitochondrial dysfunction in ASD, including chromosomal abnormalities, mitochondrial DNA mutations and large-scale deletions, and mutations in both mitochondrial and non-mitochondrial nuclear genes. Mitochondrial dysfunction has been described in immune and buccal cells, fibroblasts, muscle and gastrointestinal tissue and the brains of individuals with ASD. Several environmental factors, including toxicants, microbiome metabolites and an oxidized microenvironment are shown to modulate mitochondrial function in ASD tissues. Investigations of treatments for mitochondrial dysfunction in ASD are promising but preliminary. The etiology of mitochondrial dysfunction and how to define it in ASD is currently unclear. However, preliminary evidence suggests that the mitochondria may be a fruitful target for treatment and prevention of ASD. Further research is needed to better understand the role of mitochondrial dysfunction in the pathophysiology of ASD.

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          Synaptic, transcriptional, and chromatin genes disrupted in autism

          Silvia De Rubeis, Xin Yi He, Arthur P Goldberg (2014)
          Summary The genetic architecture of autism spectrum disorder involves the interplay of common and rare variation and their impact on hundreds of genes. Using exome sequencing, analysis of rare coding variation in 3,871 autism cases and 9,937 ancestry-matched or parental controls implicates 22 autosomal genes at a false discovery rate (FDR) < 0.05, and a set of 107 autosomal genes strongly enriched for those likely to affect risk (FDR < 0.30). These 107 genes, which show unusual evolutionary constraint against mutations, incur de novo loss-of-function mutations in over 5% of autistic subjects. Many of the genes implicated encode proteins for synaptic, transcriptional, and chromatin remodeling pathways. These include voltage-gated ion channels regulating propagation of action potentials, pacemaking, and excitability-transcription coupling, as well as histone-modifying enzymes and chromatin remodelers, prominently histone post-translational modifications involving lysine methylation/demethylation.
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            Advances in autism genetics: on the threshold of a new neurobiology.

            Brett Abrahams, Daniel Geschwind (2008)
            Autism is a heterogeneous syndrome defined by impairments in three core domains: social interaction, language and range of interests. Recent work has led to the identification of several autism susceptibility genes and an increased appreciation of the contribution of de novo and inherited copy number variation. Promising strategies are also being applied to identify common genetic risk variants. Systems biology approaches, including array-based expression profiling, are poised to provide additional insights into this group of disorders, in which heterogeneity, both genetic and phenotypic, is emerging as a dominant theme.
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              Mitochondria in the regulation of innate and adaptive immunity.

              Samuel Weinberg, Laura Sena, Navdeep Chandel (2015)
              Mitochondria are well appreciated for their role as biosynthetic and bioenergetic organelles. In the past two decades, mitochondria have emerged as signaling organelles that contribute critical decisions about cell proliferation, death, and differentiation. Mitochondria not only sustain immune cell phenotypes but also are necessary for establishing immune cell phenotype and their function. Mitochondria can rapidly switch from primarily being catabolic organelles generating ATP to anabolic organelles that generate both ATP and building blocks for macromolecule synthesis. This enables them to fulfill appropriate metabolic demands of different immune cells. Mitochondria have multiple mechanisms that allow them to activate signaling pathways in the cytosol including altering in AMP/ATP ratio, the release of ROS and TCA cycle metabolites, as well as the localization of immune regulatory proteins on the outer mitochondrial membrane. In this Review, we discuss the evidence and mechanisms that mitochondrial dependent signaling controls innate and adaptive immune responses.
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                Author and article information

                Contributors
                Richard E. Frye: rfrye@phoenixchildrens.com
                Journal
                Journal ID (nlm-ta): Mol Diagn Ther
                Journal ID (iso-abbrev): Mol Diagn Ther
                Title: Molecular Diagnosis & Therapy
                Publisher: Springer International Publishing (Cham )
                ISSN (Print): 1177-1062
                ISSN (Electronic): 1179-2000
                Publication date (Electronic): 23 July 2018
                Publication date PMC-release: 23 July 2018
                Publication date (Print): 2018
                Volume: 22
                Issue: 5
                Pages: 571-593
                Affiliations
                [1 ]ISNI 0000 0004 4687 1637, GRID grid.241054.6, Department of Pediatrics, , University of Arkansas for Medical Sciences and Arkansas Children’s Research Institute, ; Little Rock, AR USA
                [2 ]ISNI 0000 0001 0229 4979, GRID grid.416735.2, Section of Medical Genetics, , Ochsner Health System, ; New Orleans, LA USA
                [3 ]Rossignol Medical Center, Aliso Viejo, CA USA
                [4 ]ISNI 0000 0001 2181 3113, GRID grid.166341.7, Department of Pediatrics, Neurology Section, St. Christopher’s Hospital for Children, , Drexel University College of Medicine, ; Philadelphia, PA USA
                [5 ]ISNI 0000 0001 0381 0779, GRID grid.417276.1, Division of Neurodevelopmental Disorders, Department of Neurology, Barrow Neurological Institute, , Phoenix Children’s Hospital, ; 1919 E Thomas St, Phoenix, AZ USA
                [6 ]ISNI 0000 0001 2168 186X, GRID grid.134563.6, Department of Child Health, , University of Arizona College of Medicine-Phoenix, ; Phoenix, AZ USA
                Article
                Publisher ID: 352
                DOI: 10.1007/s40291-018-0352-x
                PMC ID: 6132446
                PubMed ID: 30039193
                SO-VID: 709c27db-c21b-4310-b35c-47be5a8b201a
                Copyright © © The Author(s) 2018
                License:

                Open AccessThis article is distributed under the terms of the Creative Commons Attribution-NonCommercial 4.0 International License (http://creativecommons.org/licenses/by-nc/4.0/), which permits any noncommercial use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.

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                Subject: Review Article
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                issue-copyright-statement © Springer Nature Switzerland AG 2018

                ScienceOpen disciplines: Molecular medicine
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                ScienceOpen disciplines: Molecular medicine

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