Exome Sequencing in 200 Intellectual Disability/Autistic Patients: New Candidates and Atypical Presentations

Intellectual disability (ID) and autism spectrum disorder (ASD) belong to neurodevelopmental disorders and occur in ~1% of the general population. Due to disease heterogeneity, identifying the etiology of ID and ASD remains challenging. Exome sequencing (ES) offers the opportunity to rapidly identif...

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Published in:Brain sciences 2021-07, Vol.11 (7), p.936
Main Authors: Valentino, Floriana, Bruno, Lucia Pia, Doddato, Gabriella, Giliberti, Annarita, Tita, Rossella, Resciniti, Sara, Fallerini, Chiara, Bruttini, Mirella, Lo Rizzo, Caterina, Mencarelli, Maria Antonietta, Mari, Francesca, Pinto, Anna Maria, Fava, Francesca, Baldassarri, Margherita, Fabbiani, Alessandra, Lamacchia, Vittoria, Benetti, Elisa, Zguro, Kristina, Furini, Simone, Renieri, Alessandra, Ariani, Francesca
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Language:English
Subjects:
Autism
autism spectrum disorder
Etiology
exome sequencing
Genomes
Intellectual disabilities
intellectual disability
Mutation
Neurodevelopmental disorders
Patients
Phenotyping
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cited_by cdi_FETCH-LOGICAL-c467t-401ec3dfc6fcc335c29455ba54f146c4bd0e72b149175511be8110d88c2b05ce3
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creator Valentino, Floriana
Bruno, Lucia Pia
Doddato, Gabriella
Giliberti, Annarita
Tita, Rossella
Resciniti, Sara
Fallerini, Chiara
Bruttini, Mirella
Lo Rizzo, Caterina
Mencarelli, Maria Antonietta
Mari, Francesca
Pinto, Anna Maria
Fava, Francesca
Baldassarri, Margherita
Fabbiani, Alessandra
Lamacchia, Vittoria
Benetti, Elisa
Zguro, Kristina
Furini, Simone
Renieri, Alessandra
Ariani, Francesca
description Intellectual disability (ID) and autism spectrum disorder (ASD) belong to neurodevelopmental disorders and occur in ~1% of the general population. Due to disease heterogeneity, identifying the etiology of ID and ASD remains challenging. Exome sequencing (ES) offers the opportunity to rapidly identify variants associated with these two entities that often co-exist. Here, we performed ES in a cohort of 200 patients: 84 with isolated ID and 116 with ID and ASD. We identified 41 pathogenic variants with a detection rate of 22% (43/200): 39% in ID patients (33/84) and 9% in ID/ASD patients (10/116). Most of the causative genes are genes responsible for well-established genetic syndromes that have not been recognized for atypical phenotypic presentations. Two genes emerged as new candidates: CACNA2D1 and GPR14. In conclusion, this study reinforces the importance of ES in the diagnosis of ID/ASD and underlines that “reverse phenotyping” is fundamental to enlarge the phenotypic spectra associated with specific genes.
doi_str_mv 10.3390/brainsci11070936
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subjects Autism
autism spectrum disorder
Etiology
exome sequencing
Genomes
Intellectual disabilities
intellectual disability
Mutation
Neurodevelopmental disorders
Patients
Phenotyping
title Exome Sequencing in 200 Intellectual Disability/Autistic Patients: New Candidates and Atypical Presentations
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