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Transcriptional and Ultrastructural Analyses Suggest Novel Insights into Epithelial Barrier Impairment in Celiac Disease

Disruption of epithelial junctional complex (EJC), especially tight junctions (TJ), resulting in increased intestinal permeability, is supposed to activate the enhanced immune response to gluten and to induce the development of celiac disease (CD). This study is aimed to present the role of EJC in C...

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Autores principales: Sowińska, Agnieszka, Morsy, Yasser, Czarnowska, Elżbieta, Oralewska, Beata, Konopka, Ewa, Woynarowski, Marek, Szymańska, Sylwia, Ejmont, Maria, Scharl, Michael, Bierła, Joanna B., Wawrzyniak, Marcin, Cukrowska, Bożena
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7072847/
https://www.ncbi.nlm.nih.gov/pubmed/32102433
http://dx.doi.org/10.3390/cells9020516
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author Sowińska, Agnieszka
Morsy, Yasser
Czarnowska, Elżbieta
Oralewska, Beata
Konopka, Ewa
Woynarowski, Marek
Szymańska, Sylwia
Ejmont, Maria
Scharl, Michael
Bierła, Joanna B.
Wawrzyniak, Marcin
Cukrowska, Bożena
author_facet Sowińska, Agnieszka
Morsy, Yasser
Czarnowska, Elżbieta
Oralewska, Beata
Konopka, Ewa
Woynarowski, Marek
Szymańska, Sylwia
Ejmont, Maria
Scharl, Michael
Bierła, Joanna B.
Wawrzyniak, Marcin
Cukrowska, Bożena
author_sort Sowińska, Agnieszka
collection PubMed
description Disruption of epithelial junctional complex (EJC), especially tight junctions (TJ), resulting in increased intestinal permeability, is supposed to activate the enhanced immune response to gluten and to induce the development of celiac disease (CD). This study is aimed to present the role of EJC in CD pathogenesis. To analyze differentially expressed genes the next-generation mRNA sequencing data from CD326+ epithelial cells isolated from non-celiac and celiac patients were involved. Ultrastructural studies with morphometry of EJC were done in potential CD, newly recognized active CD, and non-celiac controls. The transcriptional analysis suggested disturbances of epithelium and the most significant gene ontology enriched terms in epithelial cells from CD patients related to the plasma membrane, extracellular exome, extracellular region, and extracellular space. Ultrastructural analyses showed significantly tighter TJ, anomalies in desmosomes, dilatations of intercellular space, and shorter microvilli in potential and active CD compared to controls. Enterocytes of fetal-like type and significantly wider adherence junctions were observed only in active CD. In conclusion, the results do not support the hypothesis that an increased passage of gluten peptides by unsealing TJ precedes CD development. However, increased intestinal permeability due to abnormality of epithelium might play a role in CD onset.
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spelling pubmed-70728472020-03-19 Transcriptional and Ultrastructural Analyses Suggest Novel Insights into Epithelial Barrier Impairment in Celiac Disease Sowińska, Agnieszka Morsy, Yasser Czarnowska, Elżbieta Oralewska, Beata Konopka, Ewa Woynarowski, Marek Szymańska, Sylwia Ejmont, Maria Scharl, Michael Bierła, Joanna B. Wawrzyniak, Marcin Cukrowska, Bożena Cells Article Disruption of epithelial junctional complex (EJC), especially tight junctions (TJ), resulting in increased intestinal permeability, is supposed to activate the enhanced immune response to gluten and to induce the development of celiac disease (CD). This study is aimed to present the role of EJC in CD pathogenesis. To analyze differentially expressed genes the next-generation mRNA sequencing data from CD326+ epithelial cells isolated from non-celiac and celiac patients were involved. Ultrastructural studies with morphometry of EJC were done in potential CD, newly recognized active CD, and non-celiac controls. The transcriptional analysis suggested disturbances of epithelium and the most significant gene ontology enriched terms in epithelial cells from CD patients related to the plasma membrane, extracellular exome, extracellular region, and extracellular space. Ultrastructural analyses showed significantly tighter TJ, anomalies in desmosomes, dilatations of intercellular space, and shorter microvilli in potential and active CD compared to controls. Enterocytes of fetal-like type and significantly wider adherence junctions were observed only in active CD. In conclusion, the results do not support the hypothesis that an increased passage of gluten peptides by unsealing TJ precedes CD development. However, increased intestinal permeability due to abnormality of epithelium might play a role in CD onset. MDPI 2020-02-24 /pmc/articles/PMC7072847/ /pubmed/32102433 http://dx.doi.org/10.3390/cells9020516 Text en © 2020 by the authors. 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 (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Sowińska, Agnieszka
Morsy, Yasser
Czarnowska, Elżbieta
Oralewska, Beata
Konopka, Ewa
Woynarowski, Marek
Szymańska, Sylwia
Ejmont, Maria
Scharl, Michael
Bierła, Joanna B.
Wawrzyniak, Marcin
Cukrowska, Bożena
Transcriptional and Ultrastructural Analyses Suggest Novel Insights into Epithelial Barrier Impairment in Celiac Disease
title Transcriptional and Ultrastructural Analyses Suggest Novel Insights into Epithelial Barrier Impairment in Celiac Disease
title_full Transcriptional and Ultrastructural Analyses Suggest Novel Insights into Epithelial Barrier Impairment in Celiac Disease
title_fullStr Transcriptional and Ultrastructural Analyses Suggest Novel Insights into Epithelial Barrier Impairment in Celiac Disease
title_full_unstemmed Transcriptional and Ultrastructural Analyses Suggest Novel Insights into Epithelial Barrier Impairment in Celiac Disease
title_short Transcriptional and Ultrastructural Analyses Suggest Novel Insights into Epithelial Barrier Impairment in Celiac Disease
title_sort transcriptional and ultrastructural analyses suggest novel insights into epithelial barrier impairment in celiac disease
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7072847/
https://www.ncbi.nlm.nih.gov/pubmed/32102433
http://dx.doi.org/10.3390/cells9020516
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