Whole Exome Sequencing Is the Preferred Strategy to Identify the Genetic Defect in Patients With a Probable or Possible Mitochondrial Cause

Mitochondrial disorders, characterized by clinical symptoms and/or OXPHOS deficiencies, are caused by pathogenic variants in mitochondrial genes. However, pathogenic variants in some of these genes can lead to clinical manifestations which overlap with other neuromuscular diseases, which can be caus...

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Autores principales: Theunissen, Tom E. J., Nguyen, Minh, Kamps, Rick, Hendrickx, Alexandra T., Sallevelt, Suzanne C. E. H., Gottschalk, Ralph W. H., Calis, Chantal M., Stassen, Alphons P. M., de Koning, Bart, Mulder-Den Hartog, Elvira N. M., Schoonderwoerd, Kees, Fuchs, Sabine A., Hilhorst-Hofstee, Yvonne, de Visser, Marianne, Vanoevelen, Jo, Szklarczyk, Radek, Gerards, Mike, de Coo, Irenaeus F. M., Hellebrekers, Debby M. E. I., Smeets, Hubert J. M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2018
Materias:
Genetics
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6194163/
https://www.ncbi.nlm.nih.gov/pubmed/30369941
http://dx.doi.org/10.3389/fgene.2018.00400
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author Theunissen, Tom E. J.
Nguyen, Minh
Kamps, Rick
Hendrickx, Alexandra T.
Sallevelt, Suzanne C. E. H.
Gottschalk, Ralph W. H.
Calis, Chantal M.
Stassen, Alphons P. M.
de Koning, Bart
Mulder-Den Hartog, Elvira N. M.
Schoonderwoerd, Kees
Fuchs, Sabine A.
Hilhorst-Hofstee, Yvonne
de Visser, Marianne
Vanoevelen, Jo
Szklarczyk, Radek
Gerards, Mike
de Coo, Irenaeus F. M.
Hellebrekers, Debby M. E. I.
Smeets, Hubert J. M.
author_facet Theunissen, Tom E. J.
Nguyen, Minh
Kamps, Rick
Hendrickx, Alexandra T.
Sallevelt, Suzanne C. E. H.
Gottschalk, Ralph W. H.
Calis, Chantal M.
Stassen, Alphons P. M.
de Koning, Bart
Mulder-Den Hartog, Elvira N. M.
Schoonderwoerd, Kees
Fuchs, Sabine A.
Hilhorst-Hofstee, Yvonne
de Visser, Marianne
Vanoevelen, Jo
Szklarczyk, Radek
Gerards, Mike
de Coo, Irenaeus F. M.
Hellebrekers, Debby M. E. I.
Smeets, Hubert J. M.
author_sort Theunissen, Tom E. J.
collection PubMed
description Mitochondrial disorders, characterized by clinical symptoms and/or OXPHOS deficiencies, are caused by pathogenic variants in mitochondrial genes. However, pathogenic variants in some of these genes can lead to clinical manifestations which overlap with other neuromuscular diseases, which can be caused by pathogenic variants in non-mitochondrial genes as well. Mitochondrial pathogenic variants can be found in the mitochondrial DNA (mtDNA) or in any of the 1,500 nuclear genes with a mitochondrial function. We have performed a two-step next-generation sequencing approach in a cohort of 117 patients, mostly children, in whom a mitochondrial disease-cause could likely or possibly explain the phenotype. A total of 86 patients had a mitochondrial disorder, according to established clinical and biochemical criteria. The other 31 patients had neuromuscular symptoms, where in a minority a mitochondrial genetic cause is present, but a non-mitochondrial genetic cause is more likely. All patients were screened for pathogenic variants in the mtDNA and, if excluded, analyzed by whole exome sequencing (WES). Variants were filtered for being pathogenic and compatible with an autosomal or X-linked recessive mode of inheritance in families with multiple affected siblings and/or consanguineous parents. Non-consanguineous families with a single patient were additionally screened for autosomal and X-linked dominant mutations in a predefined gene-set. We identified causative pathogenic variants in the mtDNA in 20% of the patient-cohort, and in nuclear genes in 49%, implying an overall yield of 68%. We identified pathogenic variants in mitochondrial and non-mitochondrial genes in both groups with, obviously, a higher number of mitochondrial genes affected in mitochondrial disease patients. Furthermore, we show that 31% of the disease-causing genes in the mitochondrial patient group were not included in the MitoCarta database, and therefore would have been missed with MitoCarta based gene-panels. We conclude that WES is preferable to panel-based approaches for both groups of patients, as the mitochondrial gene-list is not complete and mitochondrial symptoms can be secondary. Also, clinically and genetically heterogeneous disorders would require sequential use of multiple different gene panels. We conclude that WES is a comprehensive and unbiased approach to establish a genetic diagnosis in these patients, able to resolve multi-genic disease-causes.
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spelling pubmed-61941632018-10-26 Whole Exome Sequencing Is the Preferred Strategy to Identify the Genetic Defect in Patients With a Probable or Possible Mitochondrial Cause Theunissen, Tom E. J. Nguyen, Minh Kamps, Rick Hendrickx, Alexandra T. Sallevelt, Suzanne C. E. H. Gottschalk, Ralph W. H. Calis, Chantal M. Stassen, Alphons P. M. de Koning, Bart Mulder-Den Hartog, Elvira N. M. Schoonderwoerd, Kees Fuchs, Sabine A. Hilhorst-Hofstee, Yvonne de Visser, Marianne Vanoevelen, Jo Szklarczyk, Radek Gerards, Mike de Coo, Irenaeus F. M. Hellebrekers, Debby M. E. I. Smeets, Hubert J. M. Front Genet Genetics Mitochondrial disorders, characterized by clinical symptoms and/or OXPHOS deficiencies, are caused by pathogenic variants in mitochondrial genes. However, pathogenic variants in some of these genes can lead to clinical manifestations which overlap with other neuromuscular diseases, which can be caused by pathogenic variants in non-mitochondrial genes as well. Mitochondrial pathogenic variants can be found in the mitochondrial DNA (mtDNA) or in any of the 1,500 nuclear genes with a mitochondrial function. We have performed a two-step next-generation sequencing approach in a cohort of 117 patients, mostly children, in whom a mitochondrial disease-cause could likely or possibly explain the phenotype. A total of 86 patients had a mitochondrial disorder, according to established clinical and biochemical criteria. The other 31 patients had neuromuscular symptoms, where in a minority a mitochondrial genetic cause is present, but a non-mitochondrial genetic cause is more likely. All patients were screened for pathogenic variants in the mtDNA and, if excluded, analyzed by whole exome sequencing (WES). Variants were filtered for being pathogenic and compatible with an autosomal or X-linked recessive mode of inheritance in families with multiple affected siblings and/or consanguineous parents. Non-consanguineous families with a single patient were additionally screened for autosomal and X-linked dominant mutations in a predefined gene-set. We identified causative pathogenic variants in the mtDNA in 20% of the patient-cohort, and in nuclear genes in 49%, implying an overall yield of 68%. We identified pathogenic variants in mitochondrial and non-mitochondrial genes in both groups with, obviously, a higher number of mitochondrial genes affected in mitochondrial disease patients. Furthermore, we show that 31% of the disease-causing genes in the mitochondrial patient group were not included in the MitoCarta database, and therefore would have been missed with MitoCarta based gene-panels. We conclude that WES is preferable to panel-based approaches for both groups of patients, as the mitochondrial gene-list is not complete and mitochondrial symptoms can be secondary. Also, clinically and genetically heterogeneous disorders would require sequential use of multiple different gene panels. We conclude that WES is a comprehensive and unbiased approach to establish a genetic diagnosis in these patients, able to resolve multi-genic disease-causes. Frontiers Media S.A. 2018-10-12 /pmc/articles/PMC6194163/ /pubmed/30369941 http://dx.doi.org/10.3389/fgene.2018.00400 Text en Copyright © 2018 Theunissen, Nguyen, Kamps, Hendrickx, Sallevelt, Gottschalk, Calis, Stassen, de Koning, Mulder-Den Hartog, Schoonderwoerd, Fuchs, Hilhorst-Hofstee, de Visser, Vanoevelen, Szklarczyk, Gerards, de Coo, Hellebrekers and Smeets. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Genetics
Theunissen, Tom E. J.
Nguyen, Minh
Kamps, Rick
Hendrickx, Alexandra T.
Sallevelt, Suzanne C. E. H.
Gottschalk, Ralph W. H.
Calis, Chantal M.
Stassen, Alphons P. M.
de Koning, Bart
Mulder-Den Hartog, Elvira N. M.
Schoonderwoerd, Kees
Fuchs, Sabine A.
Hilhorst-Hofstee, Yvonne
de Visser, Marianne
Vanoevelen, Jo
Szklarczyk, Radek
Gerards, Mike
de Coo, Irenaeus F. M.
Hellebrekers, Debby M. E. I.
Smeets, Hubert J. M.
Whole Exome Sequencing Is the Preferred Strategy to Identify the Genetic Defect in Patients With a Probable or Possible Mitochondrial Cause
title Whole Exome Sequencing Is the Preferred Strategy to Identify the Genetic Defect in Patients With a Probable or Possible Mitochondrial Cause
title_full Whole Exome Sequencing Is the Preferred Strategy to Identify the Genetic Defect in Patients With a Probable or Possible Mitochondrial Cause
title_fullStr Whole Exome Sequencing Is the Preferred Strategy to Identify the Genetic Defect in Patients With a Probable or Possible Mitochondrial Cause
title_full_unstemmed Whole Exome Sequencing Is the Preferred Strategy to Identify the Genetic Defect in Patients With a Probable or Possible Mitochondrial Cause
title_short Whole Exome Sequencing Is the Preferred Strategy to Identify the Genetic Defect in Patients With a Probable or Possible Mitochondrial Cause
title_sort whole exome sequencing is the preferred strategy to identify the genetic defect in patients with a probable or possible mitochondrial cause
topic Genetics
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6194163/
https://www.ncbi.nlm.nih.gov/pubmed/30369941
http://dx.doi.org/10.3389/fgene.2018.00400
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