Orphanet Journal of Rare Diseases (Jul 2019)
Genomic imbalances defining novel intellectual disability associated loci
- Fátima Lopes,
- Fátima Torres,
- Gabriela Soares,
- Mafalda Barbosa,
- João Silva,
- Frederico Duque,
- Miguel Rocha,
- Joaquim Sá,
- Guiomar Oliveira,
- Maria João Sá,
- Teresa Temudo,
- Susana Sousa,
- Carla Marques,
- Sofia Lopes,
- Catarina Gomes,
- Gisela Barros,
- Arminda Jorge,
- Felisbela Rocha,
- Cecília Martins,
- Sandra Mesquita,
- Susana Loureiro,
- Elisa Maria Cardoso,
- Maria José Cálix,
- Andreia Dias,
- Cristina Martins,
- Céu R. Mota,
- Diana Antunes,
- Juliette Dupont,
- Sara Figueiredo,
- Sónia Figueiroa,
- Susana Gama-de-Sousa,
- Sara Cruz,
- Adriana Sampaio,
- Paul Eijk,
- Marjan M. Weiss,
- Bauke Ylstra,
- Paula Rendeiro,
- Purificação Tavares,
- Margarida Reis-Lima,
- Jorge Pinto-Basto,
- Ana Maria Fortuna,
- Patrícia Maciel
Affiliations
- Fátima Lopes
- Life and Health Sciences Research Institute (ICVS), School of Medicine, University of Minho
- Fátima Torres
- CGC Genetics
- Gabriela Soares
- Center for Medical Genetics Dr. Jacinto Magalhães, Porto Hospital Center
- Mafalda Barbosa
- Center for Medical Genetics Dr. Jacinto Magalhães, Porto Hospital Center
- João Silva
- Center for Medical Genetics Dr. Jacinto Magalhães, Porto Hospital Center
- Frederico Duque
- Unidade de Neurodesenvolvimento e Autismo do Serviço do Centro de Desenvolvimento da Criança and Centro de Investigação e Formação Clínica, Pediatric Hospital, Centro Hospitalar e Universitário de Coimbra
- Miguel Rocha
- Center for Medical Genetics Dr. Jacinto Magalhães, Porto Hospital Center
- Joaquim Sá
- CGC Genetics
- Guiomar Oliveira
- Unidade de Neurodesenvolvimento e Autismo do Serviço do Centro de Desenvolvimento da Criança and Centro de Investigação e Formação Clínica, Pediatric Hospital, Centro Hospitalar e Universitário de Coimbra
- Maria João Sá
- Center for Medical Genetics Dr. Jacinto Magalhães, Porto Hospital Center
- Teresa Temudo
- Pediatric Neurology Department, Centro Materno-Infantil Centro Hospitalar do Porto
- Susana Sousa
- Life and Health Sciences Research Institute (ICVS), School of Medicine, University of Minho
- Carla Marques
- Unidade de Neurodesenvolvimento e Autismo do Serviço do Centro de Desenvolvimento da Criança and Centro de Investigação e Formação Clínica, Pediatric Hospital, Centro Hospitalar e Universitário de Coimbra
- Sofia Lopes
- Life and Health Sciences Research Institute (ICVS), School of Medicine, University of Minho
- Catarina Gomes
- Life and Health Sciences Research Institute (ICVS), School of Medicine, University of Minho
- Gisela Barros
- Life and Health Sciences Research Institute (ICVS), School of Medicine, University of Minho
- Arminda Jorge
- Development Unit, Pediatrics Service, Hospital Centre of Cova da Beira
- Felisbela Rocha
- Department of Pediatrics, Médio Ave Hospital Center
- Cecília Martins
- Department of Pediatrics, Médio Ave Hospital Center
- Sandra Mesquita
- Development Unit, Pediatrics Service, Hospital Centre of Cova da Beira
- Susana Loureiro
- Department of Pediatrics, Hospital S. Teotónio, Tondela/Viseu Hospital Center
- Elisa Maria Cardoso
- Department of Pediatrics, Hospital S. Teotónio, Tondela/Viseu Hospital Center
- Maria José Cálix
- Department of Pediatrics, Hospital S. Teotónio, Tondela/Viseu Hospital Center
- Andreia Dias
- Department of Pediatrics, Hospital S. Teotónio, Tondela/Viseu Hospital Center
- Cristina Martins
- Neuropaediatric Unit – Garcia de Orta Hospital
- Céu R. Mota
- Pediatric and Neonatal Intensive Care, Department of Pediatrics, Porto Hospital Center
- Diana Antunes
- Department of Genetics, Hospital D. Estefânia, Lisboa-Norte Hospital Center
- Juliette Dupont
- Genetics Service, Paediatric Department, University Hospital Santa Maria
- Sara Figueiredo
- Department of Pediatrics, Médio Ave Hospital Center
- Sónia Figueiroa
- Division of Pediatric Neurology, Department of Child and Adolescent, Centro Hospitalar do Porto e Hospital de Santo António
- Susana Gama-de-Sousa
- Department of Pediatrics, Médio Ave Hospital Center
- Sara Cruz
- Neuropsychophysiology Lab, CIPsi, School of Psychology, University of Minho
- Adriana Sampaio
- Neuropsychophysiology Lab, CIPsi, School of Psychology, University of Minho
- Paul Eijk
- Department of Pathology, VU University Medical Center
- Marjan M. Weiss
- Department of Clinical Genetics, VU University Medical Center
- Bauke Ylstra
- Department of Pathology, VU University Medical Center
- Paula Rendeiro
- CGC Genetics
- Purificação Tavares
- CGC Genetics
- Margarida Reis-Lima
- Center for Medical Genetics Dr. Jacinto Magalhães, Porto Hospital Center
- Jorge Pinto-Basto
- CGC Genetics
- Ana Maria Fortuna
- Center for Medical Genetics Dr. Jacinto Magalhães, Porto Hospital Center
- Patrícia Maciel
- Life and Health Sciences Research Institute (ICVS), School of Medicine, University of Minho
- DOI
- https://doi.org/10.1186/s13023-019-1135-0
- Journal volume & issue
-
Vol. 14,
no. 1
pp. 1 – 13
Abstract
Abstract Background High resolution genome-wide copy number analysis, routinely used in clinical diagnosis for several years, retrieves new and extremely rare copy number variations (CNVs) that provide novel candidate genes contributing to disease etiology. The aim of this work was to identify novel genetic causes of neurodevelopmental disease, inferred from CNVs detected by array comparative hybridization (aCGH), in a cohort of 325 Portuguese patients with intellectual disability (ID). Results We have detected CNVs in 30.1% of the patients, of which 5.2% corresponded to novel likely pathogenic CNVs. For these 11 rare CNVs (which encompass novel ID candidate genes), we identified those most likely to be relevant, and established genotype-phenotype correlations based on detailed clinical assessment. In the case of duplications, we performed expression analysis to assess the impact of the rearrangement. Interestingly, these novel candidate genes belong to known ID-related pathways. Within the 8% of patients with CNVs in known pathogenic loci, the majority had a clinical presentation fitting the phenotype(s) described in the literature, with a few interesting exceptions that are discussed. Conclusions Identification of such rare CNVs (some of which reported for the first time in ID patients/families) contributes to our understanding of the etiology of ID and for the ever-improving diagnosis of this group of patients.
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