SLC25A42‐associated mitochondrial encephalomyopathy: Report of additional founder cases and functional characterization of a novel deletion

SLC25A42 is the main transporter of coenzyme A (CoA) into mitochondria. To date, 15 individuals have been reported to have one of two bi‐allelic homozygous missense variants in the SLC25A42 as the cause of mitochondrial encephalomyopathy, of which 14 of them were of Saudi origin and share the same f...

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Autores principales: Aldosary, Mazhor, Baselm, Shahad, Abdulrahim, Maha, Almass, Rawan, Alsagob, Maysoon, AlMasseri, Zainab, Huma, Rozeena, AlQuait, Laila, Al‐Shidi, Tarfa, Al‐Obeid, Eman, AlBakheet, Albandary, Alahideb, Basma, Alahaidib, Lujane, Qari, Alya, Taylor, Robert W., Colak, Dilek, AlSayed, Moeenaldeen D., Kaya, Namik
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley & Sons, Inc. 2021
Materias:
Research Reports
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8260478/
https://www.ncbi.nlm.nih.gov/pubmed/34258143
http://dx.doi.org/10.1002/jmd2.12218
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author Aldosary, Mazhor
Baselm, Shahad
Abdulrahim, Maha
Almass, Rawan
Alsagob, Maysoon
AlMasseri, Zainab
Huma, Rozeena
AlQuait, Laila
Al‐Shidi, Tarfa
Al‐Obeid, Eman
AlBakheet, Albandary
Alahideb, Basma
Alahaidib, Lujane
Qari, Alya
Taylor, Robert W.
Colak, Dilek
AlSayed, Moeenaldeen D.
Kaya, Namik
author_facet Aldosary, Mazhor
Baselm, Shahad
Abdulrahim, Maha
Almass, Rawan
Alsagob, Maysoon
AlMasseri, Zainab
Huma, Rozeena
AlQuait, Laila
Al‐Shidi, Tarfa
Al‐Obeid, Eman
AlBakheet, Albandary
Alahideb, Basma
Alahaidib, Lujane
Qari, Alya
Taylor, Robert W.
Colak, Dilek
AlSayed, Moeenaldeen D.
Kaya, Namik
author_sort Aldosary, Mazhor
collection PubMed
description SLC25A42 is the main transporter of coenzyme A (CoA) into mitochondria. To date, 15 individuals have been reported to have one of two bi‐allelic homozygous missense variants in the SLC25A42 as the cause of mitochondrial encephalomyopathy, of which 14 of them were of Saudi origin and share the same founder variant, c.871A > G:p.Asn291Asp. The other subject was of German origin with a variant at canonical splice site, c.380 + 2 T > A. Here, we describe the clinical manifestations and the disease course in additional six Saudi patients from four unrelated consanguineous families. While five patients have the Saudi founder p.Asn291Asp variant, one subject has a novel deletion. Functional analyses on fibroblasts obtained from this patient revealed that the deletion causes significant decrease in mitochondrial oxygen consumption and ATP production compared to healthy individuals. Moreover, extracellular acidification rate revealed significantly reduced glycolysis, glycolytic capacity, and glycolytic reserve as compared to control individuals. There were no changes in the mitochondrial DNA (mtDNA) content of patient fibroblasts. Immunoblotting experiments revealed significantly diminished protein expression due to the deletion. In conclusion, we report additional patients with SLC25A42‐associated mitochondrial encephalomyopathy. Our study expands the molecular spectrum of this condition and provides further evidence of mitochondrial dysfunction as a central cause of pathology. We therefore propose that this disorder should be included in the differential diagnosis of any patient with an unexplained motor and speech delay, recurrent encephalopathy with metabolic acidosis, intermittent or persistent dystonia, lactic acidosis, basal ganglia lesions and, especially, of Arab ethnicity. Finally, deep brain stimulation should be considered in the management of patients with life altering dystonia.
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spelling pubmed-82604782021-07-12 SLC25A42‐associated mitochondrial encephalomyopathy: Report of additional founder cases and functional characterization of a novel deletion Aldosary, Mazhor Baselm, Shahad Abdulrahim, Maha Almass, Rawan Alsagob, Maysoon AlMasseri, Zainab Huma, Rozeena AlQuait, Laila Al‐Shidi, Tarfa Al‐Obeid, Eman AlBakheet, Albandary Alahideb, Basma Alahaidib, Lujane Qari, Alya Taylor, Robert W. Colak, Dilek AlSayed, Moeenaldeen D. Kaya, Namik JIMD Rep Research Reports SLC25A42 is the main transporter of coenzyme A (CoA) into mitochondria. To date, 15 individuals have been reported to have one of two bi‐allelic homozygous missense variants in the SLC25A42 as the cause of mitochondrial encephalomyopathy, of which 14 of them were of Saudi origin and share the same founder variant, c.871A > G:p.Asn291Asp. The other subject was of German origin with a variant at canonical splice site, c.380 + 2 T > A. Here, we describe the clinical manifestations and the disease course in additional six Saudi patients from four unrelated consanguineous families. While five patients have the Saudi founder p.Asn291Asp variant, one subject has a novel deletion. Functional analyses on fibroblasts obtained from this patient revealed that the deletion causes significant decrease in mitochondrial oxygen consumption and ATP production compared to healthy individuals. Moreover, extracellular acidification rate revealed significantly reduced glycolysis, glycolytic capacity, and glycolytic reserve as compared to control individuals. There were no changes in the mitochondrial DNA (mtDNA) content of patient fibroblasts. Immunoblotting experiments revealed significantly diminished protein expression due to the deletion. In conclusion, we report additional patients with SLC25A42‐associated mitochondrial encephalomyopathy. Our study expands the molecular spectrum of this condition and provides further evidence of mitochondrial dysfunction as a central cause of pathology. We therefore propose that this disorder should be included in the differential diagnosis of any patient with an unexplained motor and speech delay, recurrent encephalopathy with metabolic acidosis, intermittent or persistent dystonia, lactic acidosis, basal ganglia lesions and, especially, of Arab ethnicity. Finally, deep brain stimulation should be considered in the management of patients with life altering dystonia. John Wiley & Sons, Inc. 2021-05-04 /pmc/articles/PMC8260478/ /pubmed/34258143 http://dx.doi.org/10.1002/jmd2.12218 Text en © 2021 The Authors. JIMD Reports published by John Wiley & Sons Ltd on behalf of SSIEM. https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Reports
Aldosary, Mazhor
Baselm, Shahad
Abdulrahim, Maha
Almass, Rawan
Alsagob, Maysoon
AlMasseri, Zainab
Huma, Rozeena
AlQuait, Laila
Al‐Shidi, Tarfa
Al‐Obeid, Eman
AlBakheet, Albandary
Alahideb, Basma
Alahaidib, Lujane
Qari, Alya
Taylor, Robert W.
Colak, Dilek
AlSayed, Moeenaldeen D.
Kaya, Namik
SLC25A42‐associated mitochondrial encephalomyopathy: Report of additional founder cases and functional characterization of a novel deletion
title SLC25A42‐associated mitochondrial encephalomyopathy: Report of additional founder cases and functional characterization of a novel deletion
title_full SLC25A42‐associated mitochondrial encephalomyopathy: Report of additional founder cases and functional characterization of a novel deletion
title_fullStr SLC25A42‐associated mitochondrial encephalomyopathy: Report of additional founder cases and functional characterization of a novel deletion
title_full_unstemmed SLC25A42‐associated mitochondrial encephalomyopathy: Report of additional founder cases and functional characterization of a novel deletion
title_short SLC25A42‐associated mitochondrial encephalomyopathy: Report of additional founder cases and functional characterization of a novel deletion
title_sort slc25a42‐associated mitochondrial encephalomyopathy: report of additional founder cases and functional characterization of a novel deletion
topic Research Reports
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8260478/
https://www.ncbi.nlm.nih.gov/pubmed/34258143
http://dx.doi.org/10.1002/jmd2.12218
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