The Microenvironment in Barrett’s Esophagus Tissue Is Characterized by High FOXP3 and RALDH2 Levels

The Microenvironment in Barrett’s Esophagus Tissue Is Characterized by High FOXP3 and RALDH2 Levels

Metaplasia in Barrett’s esophagus (BE) is characterized by the transition of squamous epithelium into intestinal-type columnar epithelium. The immune response in BE shares many similarities with the response found in the gut, which is different from the response found in a normal-looking esophagus....

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Main Authors: Alexandra Lind, Peter D. Siersema, Johannes G. Kusters, Tanja Konijn, Reina E. Mebius, Leo Koenderman
Format: Article
Language:English
Published: Frontiers Media S.A. 2018-06-01
Series:Frontiers in Immunology
Subjects:
Barrett’s esophagus
retinoic acid
RALDH2
duodenum
reflux esophagitis
FOXP3
Online Access:https://www.frontiersin.org/article/10.3389/fimmu.2018.01375/full
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spelling doaj-bbaa39637e9b445cac49f2d359d3bb422020-11-25T01:27:31ZengFrontiers Media S.A.Frontiers in Immunology1664-32242018-06-01910.3389/fimmu.2018.01375353849The Microenvironment in Barrett’s Esophagus Tissue Is Characterized by High FOXP3 and RALDH2 LevelsAlexandra Lind0Alexandra Lind1Peter D. Siersema2Johannes G. Kusters3Tanja Konijn4Reina E. Mebius5Leo Koenderman6Laboratory of Translational Immunology, Department of Respiratory Medicine, University Medical Center Utrecht, Utrecht, NetherlandsDepartment of Gastroenterology and Hepatology, University Medical Center Utrecht, Utrecht, NetherlandsDepartment of Gastroenterology and Hepatology, University Medical Center Utrecht, Utrecht, NetherlandsDepartment of Medical Microbiology, University Medical Center Utrecht, Utrecht, NetherlandsDepartment of Molecular Cell Biology and Immunology, VU University Medical Center, Amsterdam, NetherlandsDepartment of Molecular Cell Biology and Immunology, VU University Medical Center, Amsterdam, NetherlandsLaboratory of Translational Immunology, Department of Respiratory Medicine, University Medical Center Utrecht, Utrecht, NetherlandsMetaplasia in Barrett’s esophagus (BE) is characterized by the transition of squamous epithelium into intestinal-type columnar epithelium. The immune response in BE shares many similarities with the response found in the gut, which is different from the response found in a normal-looking esophagus. Here, we investigated the role of the genes associated with the retinoic acid (RA) pathway in BE, as RA is important not only in shaping the gut’s immune response but also in the induction of metaplasia in vitro. mRNA was isolated from esophageal and duodenal biopsies from BE (n = 14), reflux esophagitis patients (n = 9), and controls (n = 12). cDNA was made and qPCR was performed. The expression of RALDH1, CYP26A1, MAdCAM1 were similar for both the BE and duodenum, but different when compared to squamous esophageal epithelium. BE was characterized by a higher expression of RALDH2 and FOXP3, compared to the duodenum. In BE, RALDH2 correlated with expression of the myeloid dendritic cell-specific genes: CD11c and CD1c. Also, RALDH2 expression correlated with RAR-β and FOXP3. Hierarchical clustering on the expression of multiple relevant genes demonstrated that BE, duodenum, and SQ tissues are clustered as three different groups. The differential expression of RA-specific genes and dendritic cell (DC)-subsets indicates that BE resembles duodenal tissue. The higher expression of RALDH2 and FOXP3 in BE points at a mechanism associated with a possible anti-inflammatory microenvironment. This aberrant immune regulation might contribute to the altered tissue and immune responses found in BE.https://www.frontiersin.org/article/10.3389/fimmu.2018.01375/fullBarrett’s esophagusretinoic acidRALDH2duodenumreflux esophagitisFOXP3
collection DOAJ
language English
format Article
sources DOAJ
author Alexandra Lind
Alexandra Lind
Peter D. Siersema
Johannes G. Kusters
Tanja Konijn
Reina E. Mebius
Leo Koenderman
spellingShingle Alexandra Lind
Alexandra Lind
Peter D. Siersema
Johannes G. Kusters
Tanja Konijn
Reina E. Mebius
Leo Koenderman
The Microenvironment in Barrett’s Esophagus Tissue Is Characterized by High FOXP3 and RALDH2 Levels
Frontiers in Immunology
Barrett’s esophagus
retinoic acid
RALDH2
duodenum
reflux esophagitis
FOXP3
author_facet Alexandra Lind
Alexandra Lind
Peter D. Siersema
Johannes G. Kusters
Tanja Konijn
Reina E. Mebius
Leo Koenderman
author_sort Alexandra Lind
title The Microenvironment in Barrett’s Esophagus Tissue Is Characterized by High FOXP3 and RALDH2 Levels
title_short The Microenvironment in Barrett’s Esophagus Tissue Is Characterized by High FOXP3 and RALDH2 Levels
title_full The Microenvironment in Barrett’s Esophagus Tissue Is Characterized by High FOXP3 and RALDH2 Levels
title_fullStr The Microenvironment in Barrett’s Esophagus Tissue Is Characterized by High FOXP3 and RALDH2 Levels
title_full_unstemmed The Microenvironment in Barrett’s Esophagus Tissue Is Characterized by High FOXP3 and RALDH2 Levels
title_sort microenvironment in barrett’s esophagus tissue is characterized by high foxp3 and raldh2 levels
publisher Frontiers Media S.A.
series Frontiers in Immunology
issn 1664-3224
publishDate 2018-06-01
description Metaplasia in Barrett’s esophagus (BE) is characterized by the transition of squamous epithelium into intestinal-type columnar epithelium. The immune response in BE shares many similarities with the response found in the gut, which is different from the response found in a normal-looking esophagus. Here, we investigated the role of the genes associated with the retinoic acid (RA) pathway in BE, as RA is important not only in shaping the gut’s immune response but also in the induction of metaplasia in vitro. mRNA was isolated from esophageal and duodenal biopsies from BE (n = 14), reflux esophagitis patients (n = 9), and controls (n = 12). cDNA was made and qPCR was performed. The expression of RALDH1, CYP26A1, MAdCAM1 were similar for both the BE and duodenum, but different when compared to squamous esophageal epithelium. BE was characterized by a higher expression of RALDH2 and FOXP3, compared to the duodenum. In BE, RALDH2 correlated with expression of the myeloid dendritic cell-specific genes: CD11c and CD1c. Also, RALDH2 expression correlated with RAR-β and FOXP3. Hierarchical clustering on the expression of multiple relevant genes demonstrated that BE, duodenum, and SQ tissues are clustered as three different groups. The differential expression of RA-specific genes and dendritic cell (DC)-subsets indicates that BE resembles duodenal tissue. The higher expression of RALDH2 and FOXP3 in BE points at a mechanism associated with a possible anti-inflammatory microenvironment. This aberrant immune regulation might contribute to the altered tissue and immune responses found in BE.
topic Barrett’s esophagus
retinoic acid
RALDH2
duodenum
reflux esophagitis
FOXP3
url https://www.frontiersin.org/article/10.3389/fimmu.2018.01375/full
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