Your browser doesn't support javascript.
loading
Genetic variability in sporadic amyotrophic lateral sclerosis.
Van Daele, Sien Hilde; Moisse, Matthieu; van Vugt, Joke J F A; Zwamborn, Ramona A J; van der Spek, Rick; van Rheenen, Wouter; Van Eijk, Kristel; Kenna, Kevin; Corcia, Philippe; Vourc'h, Patrick; Couratier, Philippe; Hardiman, Orla; McLaughin, Russell; Gotkine, Marc; Drory, Vivian; Ticozzi, Nicola; Silani, Vincenzo; Ratti, Antonia; de Carvalho, Mamede; Mora Pardina, Jesús S; Povedano, Monica; Andersen, Peter M; Weber, Markus; Basak, Nazli A; Shaw, Chris; Shaw, Pamela J; Morrison, Karen E; Landers, John E; Glass, Jonathan D; van Es, Michael A; van den Berg, Leonard H; Al-Chalabi, Ammar; Veldink, Jan; Van Damme, Philip.
Afiliação
  • Van Daele SH; Department of Neurosciences, Experimental Neurology, KU Leuven-University of Leuven, and Leuven Institute for Neuroscience and Disease (LIND), 3000 Leuven, Belgium.
  • Moisse M; VIB, Center for Brain & Disease Research, Laboratory of Neurobiology, 3000 Leuven, Belgium.
  • van Vugt JJFA; Department of Neurology, University Hospitals Leuven, 3000 Leuven, Belgium.
  • Zwamborn RAJ; Department of Human genetics, University Hospitals Leuven, 3000 Leuven, Belgium.
  • van der Spek R; Department of Neurosciences, Experimental Neurology, KU Leuven-University of Leuven, and Leuven Institute for Neuroscience and Disease (LIND), 3000 Leuven, Belgium.
  • van Rheenen W; VIB, Center for Brain & Disease Research, Laboratory of Neurobiology, 3000 Leuven, Belgium.
  • Van Eijk K; Department of Neurology, UMC Utrecht Brain Center, Utrecht University, 3584 CX Utrecht, The Netherlands.
  • Kenna K; Department of Neurology, UMC Utrecht Brain Center, Utrecht University, 3584 CX Utrecht, The Netherlands.
  • Corcia P; Department of Neurology, UMC Utrecht Brain Center, Utrecht University, 3584 CX Utrecht, The Netherlands.
  • Vourc'h P; Department of Neurology, UMC Utrecht Brain Center, Utrecht University, 3584 CX Utrecht, The Netherlands.
  • Couratier P; Department of Neurology, UMC Utrecht Brain Center, Utrecht University, 3584 CX Utrecht, The Netherlands.
  • Hardiman O; Department of Neurology, UMC Utrecht Brain Center, Utrecht University, 3584 CX Utrecht, The Netherlands.
  • McLaughin R; Centre SLA, CHRU de Tours, 37044 Tours, France.
  • Gotkine M; UMR 1253, iBrain, Université de Tours, Inserm, 37032 Tours, France.
  • Drory V; UMR 1253, iBrain, Université de Tours, Inserm, 37032 Tours, France.
  • Ticozzi N; Centre SLA, CHU Limoges, 87042 Limoges, France.
  • Silani V; Academic Unit of Neurology, Trinity College Dublin, Trinity Biomedical Sciences Institute, Dublin D02 PN40, Republic of Ireland.
  • Ratti A; Complex Trait Genomics Laboratory, Smurfit Institute of Genetics, Trinity College Dublin, Dublin D02 PN40, Republic of Ireland.
  • de Carvalho M; The Agnes Ginges Center for Human Neurogenetics, Hadassah Medical Organization and Faculty of Medicine, Hebrew University of Jerusalem, 91120 Jerusalem, Israel.
  • Mora Pardina JS; Department of Neurology, Tel-Aviv Sourasky Medical Centre, 64239 Tel Aviv, Israel.
  • Povedano M; Department of Neurology and Laboratory of Neuroscience, IRCCS Istituto Auxologico Italiano, 20149 Milano, Italy.
  • Andersen PM; Department of Pathophysiology and Transplantation, 'Dino Ferrari' Center, Università degli Studi di Milano, 20122 Milan, Italy.
  • Weber M; Department of Neurology and Laboratory of Neuroscience, IRCCS Istituto Auxologico Italiano, 20149 Milano, Italy.
  • Basak NA; Department of Pathophysiology and Transplantation, 'Dino Ferrari' Center, Università degli Studi di Milano, 20122 Milan, Italy.
  • Shaw C; Department of Neurology and Laboratory of Neuroscience, IRCCS Istituto Auxologico Italiano, 20149 Milano, Italy.
  • Shaw PJ; Department of Medical Biotechnology and Translational Medicine, Università degli Studi di Milano, 20133 Milano, Italy.
  • Morrison KE; Instituto de Fisiologia, Instituto de Medicina Molecular, Faculdade de Medicina, Universidade de Lisboa, 1649-028 Lisbon, Portugal.
  • Landers JE; ALS Unit, Hospital University San Rafael, 28016 Madrid, Spain.
  • Glass JD; Servei de Neurologia, HUB-IDIBELL, 08908 Barcelona, Spain.
  • van Es MA; Department of Clinical Science, Neurosciences, Umeå University, 901 87 Umeå, Sweden.
  • van den Berg LH; Neuromuscular Diseases Unit/ALS Clinic, Kantonsspital St. Gallen, 9007 St. Gallen, Switzerland.
  • Al-Chalabi A; Koç University, School of Medicine, KUTTAM-NDAL, 34010 Istanbul, Turkey.
  • Veldink J; Maurice Wohl Clinical Neuroscience Institute, King's College London, Department of Basic and Clinical Neuroscience, London SE5 9RT, UK.
  • Van Damme P; Sheffield Institute for Translational Neuroscience (SITraN), University of Sheffield, Sheffield S10 2HQ, UK.
Brain ; 146(9): 3760-3769, 2023 09 01.
Article em En | MEDLINE | ID: mdl-37043475
With the advent of gene therapies for amyotrophic lateral sclerosis (ALS), there is a surge in gene testing for this disease. Although there is ample experience with gene testing for C9orf72, SOD1, FUS and TARDBP in familial ALS, large studies exploring genetic variation in all ALS-associated genes in sporadic ALS (sALS) are still scarce. Gene testing in a diagnostic setting is challenging, given the complex genetic architecture of sALS, for which there are genetic variants with large and small effect sizes. Guidelines for the interpretation of genetic variants in gene panels and for counselling of patients are lacking. We aimed to provide a thorough characterization of genetic variability in ALS genes by applying the American College of Medical Genetics and Genomics (ACMG) criteria on whole genome sequencing data from a large cohort of 6013 sporadic ALS patients and 2411 matched controls from Project MinE. We studied genetic variation in 90 ALS-associated genes and applied customized ACMG-criteria to identify pathogenic and likely pathogenic variants. Variants of unknown significance were collected as well. In addition, we determined the length of repeat expansions in C9orf72, ATXN1, ATXN2 and NIPA1 using the ExpansionHunter tool. We found C9orf72 repeat expansions in 5.21% of sALS patients. In 50 ALS-associated genes, we did not identify any pathogenic or likely pathogenic variants. In 5.89%, a pathogenic or likely pathogenic variant was found, most commonly in SOD1, TARDBP, FUS, NEK1, OPTN or TBK1. Significantly more cases carried at least one pathogenic or likely pathogenic variant compared to controls (odds ratio 1.75; P-value 1.64 × 10-5). Isolated risk factors in ATXN1, ATXN2, NIPA1 and/or UNC13A were detected in 17.33% of cases. In 71.83%, we did not find any genetic clues. A combination of variants was found in 2.88%. This study provides an inventory of pathogenic and likely pathogenic genetic variation in a large cohort of sALS patients. Overall, we identified pathogenic and likely pathogenic variants in 11.13% of ALS patients in 38 known ALS genes. In line with the oligogenic hypothesis, we found significantly more combinations of variants in cases compared to controls. Many variants of unknown significance may contribute to ALS risk, but diagnostic algorithms to reliably identify and weigh them are lacking. This work can serve as a resource for counselling and for the assembly of gene panels for ALS. Further characterization of the genetic architecture of sALS is necessary given the growing interest in gene testing in ALS.
Assuntos
Palavras-chave
Texto completo
Imprimir
XML
PubMed Links
Buscar no Google

Texto completo: 1 Base de dados: MEDLINE Assunto principal: Esclerose Lateral Amiotrófica Tipo de estudo: Guideline / Prognostic_studies / Risk_factors_studies Limite: Humans País como assunto: America do norte Idioma: En Ano de publicação: 2023 Tipo de documento: Article
Texto completo
Imprimir
XML
PubMed Links
Buscar no Google

Texto completo: 1 Base de dados: MEDLINE Assunto principal: Esclerose Lateral Amiotrófica Tipo de estudo: Guideline / Prognostic_studies / Risk_factors_studies Limite: Humans País como assunto: America do norte Idioma: En Ano de publicação: 2023 Tipo de documento: Article