High genetic diagnostic yield in children and adolescents with psychiatric disorders

INTRODUCTION: Psychiatric disorders are more prevalent in children with mild (MID) to borderline intellectual functioning (BIF). Rare pathogenic variants in neurodevelopmental genes increase the risk for psychiatric disorders and may explain the comorbidity. Despite these patients represent up to 35...

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Autores principales: Manso-Bazús, C., Spataro, N., Torrent, L., Plans, L., Casadesús, M., Tomás, M., Baena, N., Trujillo, J. P., Capdevila, N., Brunet, A., Martínez-Glez, V., Pàmias, M., Ruiz Nel·lo, A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cambridge University Press 2023
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Abstract
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10595937/
http://dx.doi.org/10.1192/j.eurpsy.2023.292
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author Manso-Bazús, C.
Spataro, N.
Torrent, L.
Plans, L.
Casadesús, M.
Tomás, M.
Baena, N.
Trujillo, J. P.
Capdevila, N.
Brunet, A.
Martínez-Glez, V.
Pàmias, M.
Ruiz Nel·lo, A.
author_facet Manso-Bazús, C.
Spataro, N.
Torrent, L.
Plans, L.
Casadesús, M.
Tomás, M.
Baena, N.
Trujillo, J. P.
Capdevila, N.
Brunet, A.
Martínez-Glez, V.
Pàmias, M.
Ruiz Nel·lo, A.
author_sort Manso-Bazús, C.
collection PubMed
description INTRODUCTION: Psychiatric disorders are more prevalent in children with mild (MID) to borderline intellectual functioning (BIF). Rare pathogenic variants in neurodevelopmental genes increase the risk for psychiatric disorders and may explain the comorbidity. Despite these patients represent up to 35% of those attended at mental health services, genetic diagnosis is usually not offered. The identification of mentioned variants could lead to improved clinical care. OBJECTIVES: To identify pathogenic variants responsible of the psychiatric disorders in mild and borderline intellectual functioning. To correlate phenotypic and genetic profiles to personalize diagnostic, clinical care and support to clinicians and families. METHODS: Whole exome sequencing (WES) was performed on 99 enrolled children/adolescent (6-18 yo) affected by a psychiatric condition diagnosed following DSM-5 criteria, and either MID (IQ 55-69) or BIF (IQ 70-85). Severity and interference of IQ and psychiatric comorbidity was evaluated using several psychometric tests (Conners, CDI, STAIC, CAARMS, CBCL and hONOSCA). Inheritance pattern was assessed through Sanger sequencing. ACMG/AMP guidelines were used for variant classification. RESULTS: In our cohort, 64% patients presented BIF and 36% MID. 45% of the patients had 2 or more psychiatric diagnoses, the most prevalent (87%) being attention deficit hyperactivity disorder and, in second place, autism spectrum disorder (51%). WES identified pathogenic/likely pathogenic variants in 30% of analyzed patients (30/99), 80% of the variants were de novo. There is no significant difference in patient severity between those with a genetic diagnosis and those without. CONCLUSIONS: Rare deleterious and de novo variants in neurodevelopmental genes are responsible for the comorbidity that exists between psychiatric disorders and mild/borderline intellectual disability. The high diagnostic yield obtained from our exome sequencing approach demonstrates the need to offer genetic testing in children with psychiatric disorders and comorbid mild to borderline intellectual functioning. Finally, patients being identified with a genetic diagnosis are subsequently attended in a specialised unit for rare disorders to receive personalised clinical management. DISCLOSURE OF INTEREST: None Declared
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spelling pubmed-105959372023-10-25 High genetic diagnostic yield in children and adolescents with psychiatric disorders Manso-Bazús, C. Spataro, N. Torrent, L. Plans, L. Casadesús, M. Tomás, M. Baena, N. Trujillo, J. P. Capdevila, N. Brunet, A. Martínez-Glez, V. Pàmias, M. Ruiz Nel·lo, A. Eur Psychiatry Abstract INTRODUCTION: Psychiatric disorders are more prevalent in children with mild (MID) to borderline intellectual functioning (BIF). Rare pathogenic variants in neurodevelopmental genes increase the risk for psychiatric disorders and may explain the comorbidity. Despite these patients represent up to 35% of those attended at mental health services, genetic diagnosis is usually not offered. The identification of mentioned variants could lead to improved clinical care. OBJECTIVES: To identify pathogenic variants responsible of the psychiatric disorders in mild and borderline intellectual functioning. To correlate phenotypic and genetic profiles to personalize diagnostic, clinical care and support to clinicians and families. METHODS: Whole exome sequencing (WES) was performed on 99 enrolled children/adolescent (6-18 yo) affected by a psychiatric condition diagnosed following DSM-5 criteria, and either MID (IQ 55-69) or BIF (IQ 70-85). Severity and interference of IQ and psychiatric comorbidity was evaluated using several psychometric tests (Conners, CDI, STAIC, CAARMS, CBCL and hONOSCA). Inheritance pattern was assessed through Sanger sequencing. ACMG/AMP guidelines were used for variant classification. RESULTS: In our cohort, 64% patients presented BIF and 36% MID. 45% of the patients had 2 or more psychiatric diagnoses, the most prevalent (87%) being attention deficit hyperactivity disorder and, in second place, autism spectrum disorder (51%). WES identified pathogenic/likely pathogenic variants in 30% of analyzed patients (30/99), 80% of the variants were de novo. There is no significant difference in patient severity between those with a genetic diagnosis and those without. CONCLUSIONS: Rare deleterious and de novo variants in neurodevelopmental genes are responsible for the comorbidity that exists between psychiatric disorders and mild/borderline intellectual disability. The high diagnostic yield obtained from our exome sequencing approach demonstrates the need to offer genetic testing in children with psychiatric disorders and comorbid mild to borderline intellectual functioning. Finally, patients being identified with a genetic diagnosis are subsequently attended in a specialised unit for rare disorders to receive personalised clinical management. DISCLOSURE OF INTEREST: None Declared Cambridge University Press 2023-07-19 /pmc/articles/PMC10595937/ http://dx.doi.org/10.1192/j.eurpsy.2023.292 Text en © The Author(s) 2023 https://creativecommons.org/licenses/by/4.0/This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (https://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Abstract
Manso-Bazús, C.
Spataro, N.
Torrent, L.
Plans, L.
Casadesús, M.
Tomás, M.
Baena, N.
Trujillo, J. P.
Capdevila, N.
Brunet, A.
Martínez-Glez, V.
Pàmias, M.
Ruiz Nel·lo, A.
High genetic diagnostic yield in children and adolescents with psychiatric disorders
title High genetic diagnostic yield in children and adolescents with psychiatric disorders
title_full High genetic diagnostic yield in children and adolescents with psychiatric disorders
title_fullStr High genetic diagnostic yield in children and adolescents with psychiatric disorders
title_full_unstemmed High genetic diagnostic yield in children and adolescents with psychiatric disorders
title_short High genetic diagnostic yield in children and adolescents with psychiatric disorders
title_sort high genetic diagnostic yield in children and adolescents with psychiatric disorders
topic Abstract
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10595937/
http://dx.doi.org/10.1192/j.eurpsy.2023.292
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