Biallelic SYNE2 Missense Mutations Leading to Nesprin-2 Giant Hypo-Expression Are Associated with Intellectual Disability and Autism

Autism spectrum disorder (ASD) is a group of neurological and developmental disabilities characterised by clinical and genetic heterogeneity. The current study aimed to expand ASD genotyping by investigating potential associations with SYNE2 mutations. Specifically, the disease-causing variants of S...

Descripción completa

Detalles Bibliográficos
Autores principales: Young, Natalie, Asif, Maria, Jackson, Matthew, Fernández-Mayoralas, Daniel Martín, de la Peña, Mar Jimenez, Calleja-Pérez, Beatriz, Álvarez, Sara, Hunter-Featherstone, Eve, Noegel, Angelika A., Höhne, Wolfgang, Nürnberg, Peter, Obara, Boguslaw, Hussain, Muhammad Sajid, Karakesisoglou, Iakowos, Fernández-Jaén, Alberto
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8470961/
https://www.ncbi.nlm.nih.gov/pubmed/34573277
http://dx.doi.org/10.3390/genes12091294
_version_ 1784574334215389184
author Young, Natalie
Asif, Maria
Jackson, Matthew
Fernández-Mayoralas, Daniel Martín
de la Peña, Mar Jimenez
Calleja-Pérez, Beatriz
Álvarez, Sara
Hunter-Featherstone, Eve
Noegel, Angelika A.
Höhne, Wolfgang
Nürnberg, Peter
Obara, Boguslaw
Hussain, Muhammad Sajid
Karakesisoglou, Iakowos
Fernández-Jaén, Alberto
author_facet Young, Natalie
Asif, Maria
Jackson, Matthew
Fernández-Mayoralas, Daniel Martín
de la Peña, Mar Jimenez
Calleja-Pérez, Beatriz
Álvarez, Sara
Hunter-Featherstone, Eve
Noegel, Angelika A.
Höhne, Wolfgang
Nürnberg, Peter
Obara, Boguslaw
Hussain, Muhammad Sajid
Karakesisoglou, Iakowos
Fernández-Jaén, Alberto
author_sort Young, Natalie
collection PubMed
description Autism spectrum disorder (ASD) is a group of neurological and developmental disabilities characterised by clinical and genetic heterogeneity. The current study aimed to expand ASD genotyping by investigating potential associations with SYNE2 mutations. Specifically, the disease-causing variants of SYNE2 in 410 trios manifesting neurodevelopmental disorders using whole-exome sequencing were explored. The consequences of the identified variants were studied at the transcript level using quantitative polymerase chain reaction (qPCR). For validation, immunofluorescence and immunoblotting were performed to analyse mutational effects at the protein level. The compound heterozygous variants of SYNE2 (NM_182914.3:c.2483T>G; p.(Val828Gly) and NM_182914.3:c.2362G>A; p.(Glu788Lys)) were identified in a 4.5-year-old male, clinically diagnosed with autism spectrum disorder, developmental delay and intellectual disability. Both variants reside within the nesprin-2 giant spectrin repeat (SR5) domain and are predicted to be highly damaging using in silico tools. Specifically, a significant reduction of nesprin-2 giant protein levels is revealed in patient cells. SYNE2 transcription and the nuclear envelope localisation of the mutant proteins was however unaffected as compared to parental control cells. Collectively, these data provide novel insights into the cardinal role of the nesprin-2 giant in neurodevelopment and suggest that the biallelic hypomorphic SYNE2 mutations may be a new cause of intellectual disability and ASD.
format Online
Article
Text
id pubmed-8470961
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-84709612021-09-27 Biallelic SYNE2 Missense Mutations Leading to Nesprin-2 Giant Hypo-Expression Are Associated with Intellectual Disability and Autism Young, Natalie Asif, Maria Jackson, Matthew Fernández-Mayoralas, Daniel Martín de la Peña, Mar Jimenez Calleja-Pérez, Beatriz Álvarez, Sara Hunter-Featherstone, Eve Noegel, Angelika A. Höhne, Wolfgang Nürnberg, Peter Obara, Boguslaw Hussain, Muhammad Sajid Karakesisoglou, Iakowos Fernández-Jaén, Alberto Genes (Basel) Article Autism spectrum disorder (ASD) is a group of neurological and developmental disabilities characterised by clinical and genetic heterogeneity. The current study aimed to expand ASD genotyping by investigating potential associations with SYNE2 mutations. Specifically, the disease-causing variants of SYNE2 in 410 trios manifesting neurodevelopmental disorders using whole-exome sequencing were explored. The consequences of the identified variants were studied at the transcript level using quantitative polymerase chain reaction (qPCR). For validation, immunofluorescence and immunoblotting were performed to analyse mutational effects at the protein level. The compound heterozygous variants of SYNE2 (NM_182914.3:c.2483T>G; p.(Val828Gly) and NM_182914.3:c.2362G>A; p.(Glu788Lys)) were identified in a 4.5-year-old male, clinically diagnosed with autism spectrum disorder, developmental delay and intellectual disability. Both variants reside within the nesprin-2 giant spectrin repeat (SR5) domain and are predicted to be highly damaging using in silico tools. Specifically, a significant reduction of nesprin-2 giant protein levels is revealed in patient cells. SYNE2 transcription and the nuclear envelope localisation of the mutant proteins was however unaffected as compared to parental control cells. Collectively, these data provide novel insights into the cardinal role of the nesprin-2 giant in neurodevelopment and suggest that the biallelic hypomorphic SYNE2 mutations may be a new cause of intellectual disability and ASD. MDPI 2021-08-24 /pmc/articles/PMC8470961/ /pubmed/34573277 http://dx.doi.org/10.3390/genes12091294 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Young, Natalie
Asif, Maria
Jackson, Matthew
Fernández-Mayoralas, Daniel Martín
de la Peña, Mar Jimenez
Calleja-Pérez, Beatriz
Álvarez, Sara
Hunter-Featherstone, Eve
Noegel, Angelika A.
Höhne, Wolfgang
Nürnberg, Peter
Obara, Boguslaw
Hussain, Muhammad Sajid
Karakesisoglou, Iakowos
Fernández-Jaén, Alberto
Biallelic SYNE2 Missense Mutations Leading to Nesprin-2 Giant Hypo-Expression Are Associated with Intellectual Disability and Autism
title Biallelic SYNE2 Missense Mutations Leading to Nesprin-2 Giant Hypo-Expression Are Associated with Intellectual Disability and Autism
title_full Biallelic SYNE2 Missense Mutations Leading to Nesprin-2 Giant Hypo-Expression Are Associated with Intellectual Disability and Autism
title_fullStr Biallelic SYNE2 Missense Mutations Leading to Nesprin-2 Giant Hypo-Expression Are Associated with Intellectual Disability and Autism
title_full_unstemmed Biallelic SYNE2 Missense Mutations Leading to Nesprin-2 Giant Hypo-Expression Are Associated with Intellectual Disability and Autism
title_short Biallelic SYNE2 Missense Mutations Leading to Nesprin-2 Giant Hypo-Expression Are Associated with Intellectual Disability and Autism
title_sort biallelic syne2 missense mutations leading to nesprin-2 giant hypo-expression are associated with intellectual disability and autism
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8470961/
https://www.ncbi.nlm.nih.gov/pubmed/34573277
http://dx.doi.org/10.3390/genes12091294
work_keys_str_mv AT youngnatalie biallelicsyne2missensemutationsleadingtonesprin2gianthypoexpressionareassociatedwithintellectualdisabilityandautism
AT asifmaria biallelicsyne2missensemutationsleadingtonesprin2gianthypoexpressionareassociatedwithintellectualdisabilityandautism
AT jacksonmatthew biallelicsyne2missensemutationsleadingtonesprin2gianthypoexpressionareassociatedwithintellectualdisabilityandautism
AT fernandezmayoralasdanielmartin biallelicsyne2missensemutationsleadingtonesprin2gianthypoexpressionareassociatedwithintellectualdisabilityandautism
AT delapenamarjimenez biallelicsyne2missensemutationsleadingtonesprin2gianthypoexpressionareassociatedwithintellectualdisabilityandautism
AT callejaperezbeatriz biallelicsyne2missensemutationsleadingtonesprin2gianthypoexpressionareassociatedwithintellectualdisabilityandautism
AT alvarezsara biallelicsyne2missensemutationsleadingtonesprin2gianthypoexpressionareassociatedwithintellectualdisabilityandautism
AT hunterfeatherstoneeve biallelicsyne2missensemutationsleadingtonesprin2gianthypoexpressionareassociatedwithintellectualdisabilityandautism
AT noegelangelikaa biallelicsyne2missensemutationsleadingtonesprin2gianthypoexpressionareassociatedwithintellectualdisabilityandautism
AT hohnewolfgang biallelicsyne2missensemutationsleadingtonesprin2gianthypoexpressionareassociatedwithintellectualdisabilityandautism
AT nurnbergpeter biallelicsyne2missensemutationsleadingtonesprin2gianthypoexpressionareassociatedwithintellectualdisabilityandautism
AT obaraboguslaw biallelicsyne2missensemutationsleadingtonesprin2gianthypoexpressionareassociatedwithintellectualdisabilityandautism
AT hussainmuhammadsajid biallelicsyne2missensemutationsleadingtonesprin2gianthypoexpressionareassociatedwithintellectualdisabilityandautism
AT karakesisoglouiakowos biallelicsyne2missensemutationsleadingtonesprin2gianthypoexpressionareassociatedwithintellectualdisabilityandautism
AT fernandezjaenalberto biallelicsyne2missensemutationsleadingtonesprin2gianthypoexpressionareassociatedwithintellectualdisabilityandautism

Ejemplares similares