Mitochondrial dysfunction and autism: comprehensive genetic analyses of children with autism and mtDNA deletion

BACKGROUND: The etiology of autism spectrum disorders (ASD) is very heterogeneous. Mitochondrial dysfunction has been described in ASD; however, primary mitochondrial disease has been genetically proven in a small subset of patients. The main goal of the present study was to investigate correlations...

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Autores principales: Varga, Noémi Ágnes, Pentelényi, Klára, Balicza, Péter, Gézsi, András, Reményi, Viktória, Hársfalvi, Vivien, Bencsik, Renáta, Illés, Anett, Prekop, Csilla, Molnár, Mária Judit
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2018
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5819172/
https://www.ncbi.nlm.nih.gov/pubmed/29458409
http://dx.doi.org/10.1186/s12993-018-0135-x
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author Varga, Noémi Ágnes
Pentelényi, Klára
Balicza, Péter
Gézsi, András
Reményi, Viktória
Hársfalvi, Vivien
Bencsik, Renáta
Illés, Anett
Prekop, Csilla
Molnár, Mária Judit
author_facet Varga, Noémi Ágnes
Pentelényi, Klára
Balicza, Péter
Gézsi, András
Reményi, Viktória
Hársfalvi, Vivien
Bencsik, Renáta
Illés, Anett
Prekop, Csilla
Molnár, Mária Judit
author_sort Varga, Noémi Ágnes
collection PubMed
description BACKGROUND: The etiology of autism spectrum disorders (ASD) is very heterogeneous. Mitochondrial dysfunction has been described in ASD; however, primary mitochondrial disease has been genetically proven in a small subset of patients. The main goal of the present study was to investigate correlations between mitochondrial DNA (mtDNA) changes and alterations of genes associated with mtDNA maintenance or ASD. METHODS: Sixty patients with ASD and sixty healthy individuals were screened for common mtDNA mutations. Next generation sequencing was performed on patients with major mtDNA deletions (mtdel-ASD) using two gene panels to investigate nuclear genes that are associated with ASD or are responsible for mtDNA maintenance. Cohorts of healthy controls, ASD patients without mtDNA alterations, and patients with mitochondrial disorders (non-ASD) harbouring mtDNA deletions served as comparison groups. RESULTS: MtDNA deletions were confirmed in 16.6% (10/60) of patients with ASD (mtdel-ASD). In 90% of this mtdel-ASD children we found rare SNVs in ASD-associated genes (one of those was pathogenic). In the intergenomic panel of this cohort one likely pathogenic variant was present. In patients with mitochondrial disease in genes responsible for mtDNA maintenance pathogenic mutations and variants of uncertain significance (VUS) were detected more frequently than those found in patients from the mtdel-ASD or other comparison groups. In healthy controls and in patients without a mtDNA deletion, only VUS were detected in both panel. CONCLUSIONS: MtDNA alterations are more common in patients with ASD than in control individuals. MtDNA deletions are not isolated genetic alterations found in ASD; they coexist either with other ASD-associated genetic risk factors or with alterations in genes responsible for intergenomic communication. These findings indicate that mitochondrial dysfunction is not rare in ASD. The occurring mtDNA deletions in ASD may be mostly a consequence of the alterations of the causative culprit genes for autism or genes responsible for mtDNA maintenance, or because of the harmful effect of environmental factors. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1186/s12993-018-0135-x) contains supplementary material, which is available to authorized users.
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spelling pubmed-58191722018-02-21 Mitochondrial dysfunction and autism: comprehensive genetic analyses of children with autism and mtDNA deletion Varga, Noémi Ágnes Pentelényi, Klára Balicza, Péter Gézsi, András Reményi, Viktória Hársfalvi, Vivien Bencsik, Renáta Illés, Anett Prekop, Csilla Molnár, Mária Judit Behav Brain Funct Research BACKGROUND: The etiology of autism spectrum disorders (ASD) is very heterogeneous. Mitochondrial dysfunction has been described in ASD; however, primary mitochondrial disease has been genetically proven in a small subset of patients. The main goal of the present study was to investigate correlations between mitochondrial DNA (mtDNA) changes and alterations of genes associated with mtDNA maintenance or ASD. METHODS: Sixty patients with ASD and sixty healthy individuals were screened for common mtDNA mutations. Next generation sequencing was performed on patients with major mtDNA deletions (mtdel-ASD) using two gene panels to investigate nuclear genes that are associated with ASD or are responsible for mtDNA maintenance. Cohorts of healthy controls, ASD patients without mtDNA alterations, and patients with mitochondrial disorders (non-ASD) harbouring mtDNA deletions served as comparison groups. RESULTS: MtDNA deletions were confirmed in 16.6% (10/60) of patients with ASD (mtdel-ASD). In 90% of this mtdel-ASD children we found rare SNVs in ASD-associated genes (one of those was pathogenic). In the intergenomic panel of this cohort one likely pathogenic variant was present. In patients with mitochondrial disease in genes responsible for mtDNA maintenance pathogenic mutations and variants of uncertain significance (VUS) were detected more frequently than those found in patients from the mtdel-ASD or other comparison groups. In healthy controls and in patients without a mtDNA deletion, only VUS were detected in both panel. CONCLUSIONS: MtDNA alterations are more common in patients with ASD than in control individuals. MtDNA deletions are not isolated genetic alterations found in ASD; they coexist either with other ASD-associated genetic risk factors or with alterations in genes responsible for intergenomic communication. These findings indicate that mitochondrial dysfunction is not rare in ASD. The occurring mtDNA deletions in ASD may be mostly a consequence of the alterations of the causative culprit genes for autism or genes responsible for mtDNA maintenance, or because of the harmful effect of environmental factors. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1186/s12993-018-0135-x) contains supplementary material, which is available to authorized users. BioMed Central 2018-02-20 /pmc/articles/PMC5819172/ /pubmed/29458409 http://dx.doi.org/10.1186/s12993-018-0135-x Text en © The Author(s) 2018 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted 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. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
Varga, Noémi Ágnes
Pentelényi, Klára
Balicza, Péter
Gézsi, András
Reményi, Viktória
Hársfalvi, Vivien
Bencsik, Renáta
Illés, Anett
Prekop, Csilla
Molnár, Mária Judit
Mitochondrial dysfunction and autism: comprehensive genetic analyses of children with autism and mtDNA deletion
title Mitochondrial dysfunction and autism: comprehensive genetic analyses of children with autism and mtDNA deletion
title_full Mitochondrial dysfunction and autism: comprehensive genetic analyses of children with autism and mtDNA deletion
title_fullStr Mitochondrial dysfunction and autism: comprehensive genetic analyses of children with autism and mtDNA deletion
title_full_unstemmed Mitochondrial dysfunction and autism: comprehensive genetic analyses of children with autism and mtDNA deletion
title_short Mitochondrial dysfunction and autism: comprehensive genetic analyses of children with autism and mtDNA deletion
title_sort mitochondrial dysfunction and autism: comprehensive genetic analyses of children with autism and mtdna deletion
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5819172/
https://www.ncbi.nlm.nih.gov/pubmed/29458409
http://dx.doi.org/10.1186/s12993-018-0135-x
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