Phenotypic and functional consequences of haploinsufficiency of genes from exocyst and retinoic acid pathway due to a recurrent microdeletion of 2p13.2

BACKGROUND: Rare, recurrent genomic imbalances facilitate the association of genotype with abnormalities at the “whole body” level. However, at the cellular level, the functional consequences of recurrent genomic abnormalities and how they can be linked to the phenotype are much less investigated. M...

Descripción completa

Detalles Bibliográficos
Autores principales: Wen, Jiadi, Lopes, Fátima, Soares, Gabriela, Farrell, Sandra A, Nelson, Cara, Qiao, Ying, Martell, Sally, Badukke, Chansonette, Bessa, Carlos, Ylstra, Bauke, Lewis, Suzanne, Isoherranen, Nina, Maciel, Patricia, Rajcan-Separovic, Evica
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3710273/
https://www.ncbi.nlm.nih.gov/pubmed/23837398
http://dx.doi.org/10.1186/1750-1172-8-100
_version_ 1782276857051217920
author Wen, Jiadi
Lopes, Fátima
Soares, Gabriela
Farrell, Sandra A
Nelson, Cara
Qiao, Ying
Martell, Sally
Badukke, Chansonette
Bessa, Carlos
Ylstra, Bauke
Lewis, Suzanne
Isoherranen, Nina
Maciel, Patricia
Rajcan-Separovic, Evica
author_facet Wen, Jiadi
Lopes, Fátima
Soares, Gabriela
Farrell, Sandra A
Nelson, Cara
Qiao, Ying
Martell, Sally
Badukke, Chansonette
Bessa, Carlos
Ylstra, Bauke
Lewis, Suzanne
Isoherranen, Nina
Maciel, Patricia
Rajcan-Separovic, Evica
author_sort Wen, Jiadi
collection PubMed
description BACKGROUND: Rare, recurrent genomic imbalances facilitate the association of genotype with abnormalities at the “whole body” level. However, at the cellular level, the functional consequences of recurrent genomic abnormalities and how they can be linked to the phenotype are much less investigated. METHOD AND RESULTS: We report an example of a functional analysis of two genes from a new, overlapping microdeletion of 2p13.2 region (from 72,140,702-72,924,626). The subjects shared intellectual disability (ID), language delay, hyperactivity, facial asymmetry, ear malformations, and vertebral and/or craniofacial abnormalities. The overlapping region included two genes, EXOC6B and CYP26B1, which are involved in exocytosis/Notch signaling and retinoic acid (RA) metabolism, respectively, and are of critical importance for early morphogenesis, symmetry as well as craniofacial, skeleton and brain development. The abnormal function of EXOC6B was documented in patient lymphoblasts by its reduced expression and with perturbed expression of Notch signaling pathway genes HES1 and RBPJ, previously noted to be the consequence of EXOC6B dysfunction in animal and cell line models. Similarly, the function of CYP26B1 was affected by the deletion since the retinoic acid induced expression of this gene in patient lymphoblasts was significantly lower compared to controls (8% of controls). CONCLUSION: Haploinsufficiency of CYP26B1 and EXOC6B genes involved in retinoic acid and exocyst/Notch signaling pathways, respectively, has not been reported previously in humans. The developmental anomalies and phenotypic features of our subjects are in keeping with the dysfunction of these genes, considering their known role. Documenting their dysfunction at the cellular level in patient cells enhanced our understanding of biological processes which contribute to the clinical phenotype.
format Online
Article
Text
id pubmed-3710273
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-37102732013-07-13 Phenotypic and functional consequences of haploinsufficiency of genes from exocyst and retinoic acid pathway due to a recurrent microdeletion of 2p13.2 Wen, Jiadi Lopes, Fátima Soares, Gabriela Farrell, Sandra A Nelson, Cara Qiao, Ying Martell, Sally Badukke, Chansonette Bessa, Carlos Ylstra, Bauke Lewis, Suzanne Isoherranen, Nina Maciel, Patricia Rajcan-Separovic, Evica Orphanet J Rare Dis Research BACKGROUND: Rare, recurrent genomic imbalances facilitate the association of genotype with abnormalities at the “whole body” level. However, at the cellular level, the functional consequences of recurrent genomic abnormalities and how they can be linked to the phenotype are much less investigated. METHOD AND RESULTS: We report an example of a functional analysis of two genes from a new, overlapping microdeletion of 2p13.2 region (from 72,140,702-72,924,626). The subjects shared intellectual disability (ID), language delay, hyperactivity, facial asymmetry, ear malformations, and vertebral and/or craniofacial abnormalities. The overlapping region included two genes, EXOC6B and CYP26B1, which are involved in exocytosis/Notch signaling and retinoic acid (RA) metabolism, respectively, and are of critical importance for early morphogenesis, symmetry as well as craniofacial, skeleton and brain development. The abnormal function of EXOC6B was documented in patient lymphoblasts by its reduced expression and with perturbed expression of Notch signaling pathway genes HES1 and RBPJ, previously noted to be the consequence of EXOC6B dysfunction in animal and cell line models. Similarly, the function of CYP26B1 was affected by the deletion since the retinoic acid induced expression of this gene in patient lymphoblasts was significantly lower compared to controls (8% of controls). CONCLUSION: Haploinsufficiency of CYP26B1 and EXOC6B genes involved in retinoic acid and exocyst/Notch signaling pathways, respectively, has not been reported previously in humans. The developmental anomalies and phenotypic features of our subjects are in keeping with the dysfunction of these genes, considering their known role. Documenting their dysfunction at the cellular level in patient cells enhanced our understanding of biological processes which contribute to the clinical phenotype. BioMed Central 2013-07-10 /pmc/articles/PMC3710273/ /pubmed/23837398 http://dx.doi.org/10.1186/1750-1172-8-100 Text en Copyright © 2013 Wen et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Wen, Jiadi
Lopes, Fátima
Soares, Gabriela
Farrell, Sandra A
Nelson, Cara
Qiao, Ying
Martell, Sally
Badukke, Chansonette
Bessa, Carlos
Ylstra, Bauke
Lewis, Suzanne
Isoherranen, Nina
Maciel, Patricia
Rajcan-Separovic, Evica
Phenotypic and functional consequences of haploinsufficiency of genes from exocyst and retinoic acid pathway due to a recurrent microdeletion of 2p13.2
title Phenotypic and functional consequences of haploinsufficiency of genes from exocyst and retinoic acid pathway due to a recurrent microdeletion of 2p13.2
title_full Phenotypic and functional consequences of haploinsufficiency of genes from exocyst and retinoic acid pathway due to a recurrent microdeletion of 2p13.2
title_fullStr Phenotypic and functional consequences of haploinsufficiency of genes from exocyst and retinoic acid pathway due to a recurrent microdeletion of 2p13.2
title_full_unstemmed Phenotypic and functional consequences of haploinsufficiency of genes from exocyst and retinoic acid pathway due to a recurrent microdeletion of 2p13.2
title_short Phenotypic and functional consequences of haploinsufficiency of genes from exocyst and retinoic acid pathway due to a recurrent microdeletion of 2p13.2
title_sort phenotypic and functional consequences of haploinsufficiency of genes from exocyst and retinoic acid pathway due to a recurrent microdeletion of 2p13.2
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3710273/
https://www.ncbi.nlm.nih.gov/pubmed/23837398
http://dx.doi.org/10.1186/1750-1172-8-100
work_keys_str_mv AT wenjiadi phenotypicandfunctionalconsequencesofhaploinsufficiencyofgenesfromexocystandretinoicacidpathwayduetoarecurrentmicrodeletionof2p132
AT lopesfatima phenotypicandfunctionalconsequencesofhaploinsufficiencyofgenesfromexocystandretinoicacidpathwayduetoarecurrentmicrodeletionof2p132
AT soaresgabriela phenotypicandfunctionalconsequencesofhaploinsufficiencyofgenesfromexocystandretinoicacidpathwayduetoarecurrentmicrodeletionof2p132
AT farrellsandraa phenotypicandfunctionalconsequencesofhaploinsufficiencyofgenesfromexocystandretinoicacidpathwayduetoarecurrentmicrodeletionof2p132
AT nelsoncara phenotypicandfunctionalconsequencesofhaploinsufficiencyofgenesfromexocystandretinoicacidpathwayduetoarecurrentmicrodeletionof2p132
AT qiaoying phenotypicandfunctionalconsequencesofhaploinsufficiencyofgenesfromexocystandretinoicacidpathwayduetoarecurrentmicrodeletionof2p132
AT martellsally phenotypicandfunctionalconsequencesofhaploinsufficiencyofgenesfromexocystandretinoicacidpathwayduetoarecurrentmicrodeletionof2p132
AT badukkechansonette phenotypicandfunctionalconsequencesofhaploinsufficiencyofgenesfromexocystandretinoicacidpathwayduetoarecurrentmicrodeletionof2p132
AT bessacarlos phenotypicandfunctionalconsequencesofhaploinsufficiencyofgenesfromexocystandretinoicacidpathwayduetoarecurrentmicrodeletionof2p132
AT ylstrabauke phenotypicandfunctionalconsequencesofhaploinsufficiencyofgenesfromexocystandretinoicacidpathwayduetoarecurrentmicrodeletionof2p132
AT lewissuzanne phenotypicandfunctionalconsequencesofhaploinsufficiencyofgenesfromexocystandretinoicacidpathwayduetoarecurrentmicrodeletionof2p132
AT isoherranennina phenotypicandfunctionalconsequencesofhaploinsufficiencyofgenesfromexocystandretinoicacidpathwayduetoarecurrentmicrodeletionof2p132
AT macielpatricia phenotypicandfunctionalconsequencesofhaploinsufficiencyofgenesfromexocystandretinoicacidpathwayduetoarecurrentmicrodeletionof2p132
AT rajcanseparovicevica phenotypicandfunctionalconsequencesofhaploinsufficiencyofgenesfromexocystandretinoicacidpathwayduetoarecurrentmicrodeletionof2p132

Ejemplares similares