Interleukin‐13 and interleukin‐33 mRNA are underexpressed in the duodenal mucosa of German Shepherd dogs with chronic enteropathy

Interleukin‐13 and interleukin‐33 mRNA are underexpressed in the duodenal mucosa of German Shepherd dogs with chronic enteropathy

Abstract Background A recent genome‐wide association study in German Shepherd dogs (GSDs) with chronic enteropathy (CE) has identified polymorphisms in the Th2 cytokine genes. Hypothesis/objective To determine if the expression of the Th2 cytokines, interleukin‐13 (IL‐13) and interleukin‐33 (IL‐33),...

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Main Authors: Aarti Kathrani, Victor Lezcano, Edward J. Hall, Albert E. Jergens, Yeon‐Jung Seo, Jonathan P. Mochel, Todd Atherly, Karin Allenspach
Format: Article
Language:English
Published: Wiley 2019-07-01
Series:Journal of Veterinary Internal Medicine
Subjects:
bowel
canine
cytokine
duodenum
inflammatory
Th2
Online Access:https://doi.org/10.1111/jvim.15544
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spelling doaj-5f196b58841f4a1fb879b604f112e9752020-11-24T22:14:36ZengWileyJournal of Veterinary Internal Medicine0891-66401939-16762019-07-013341660166810.1111/jvim.15544Interleukin‐13 and interleukin‐33 mRNA are underexpressed in the duodenal mucosa of German Shepherd dogs with chronic enteropathyAarti Kathrani0Victor Lezcano1Edward J. Hall2Albert E. Jergens3Yeon‐Jung Seo4Jonathan P. Mochel5Todd Atherly6Karin Allenspach7Royal Veterinary College Hertfordshire United KingdomCollege of Veterinary Medicine Tuskegee University Tuskegee AlabamaBristol Veterinary School University of Bristol Bristol United KingdomCollege of Veterinary Medicine Iowa State University Ames IowaCollege of Veterinary Medicine Iowa State University Ames IowaCollege of Veterinary Medicine Iowa State University Ames IowaCollege of Veterinary Medicine Iowa State University Ames IowaCollege of Veterinary Medicine Iowa State University Ames IowaAbstract Background A recent genome‐wide association study in German Shepherd dogs (GSDs) with chronic enteropathy (CE) has identified polymorphisms in the Th2 cytokine genes. Hypothesis/objective To determine if the expression of the Th2 cytokines, interleukin‐13 (IL‐13) and interleukin‐33 (IL‐33), is altered in the duodenal mucosa of GSDs with CE compared to non‐GSDs with CE and healthy dogs. Animals Twenty client‐owned dogs diagnosed with CE (10 GSDs and 10 non‐GSDs) at the Bristol Veterinary School and 8 healthy Beagle dogs from the Iowa State University Service Colony. Methods Retrospective study using archived paraffin‐embedded duodenal biopsy samples. A novel RNA in situ hybridization technology (RNAscope) was used to hybridize IL‐13 and IL‐33 mRNA probes onto at least 10 sections from duodenal biopsy samples for each dog. RNAscope signals were visualized using a microscope and semi‐quantitative assessment was performed by a single operator. Results Based on duodenal villus, subvillus, epithelial, and lamina propria average expression scores, GSDs with CE had significantly lower IL‐13 and IL‐33 mRNA expression compared to non‐GSDs with CE (IL‐13, P < .04; IL‐33, P < .02) and healthy Beagle dogs (IL‐13, P < .02; IL‐33, P < .004). Conclusions and Clinical Importance Similar to human patients with ulcerative colitis, a subtype of human inflammatory bowel disease, these data indicate that Th2 cytokines may be involved in the pathogenesis of CE in GSDs.https://doi.org/10.1111/jvim.15544bowelcaninecytokineduodenuminflammatoryTh2
collection DOAJ
language English
format Article
sources DOAJ
author Aarti Kathrani
Victor Lezcano
Edward J. Hall
Albert E. Jergens
Yeon‐Jung Seo
Jonathan P. Mochel
Todd Atherly
Karin Allenspach
spellingShingle Aarti Kathrani
Victor Lezcano
Edward J. Hall
Albert E. Jergens
Yeon‐Jung Seo
Jonathan P. Mochel
Todd Atherly
Karin Allenspach
Interleukin‐13 and interleukin‐33 mRNA are underexpressed in the duodenal mucosa of German Shepherd dogs with chronic enteropathy
Journal of Veterinary Internal Medicine
bowel
canine
cytokine
duodenum
inflammatory
Th2
author_facet Aarti Kathrani
Victor Lezcano
Edward J. Hall
Albert E. Jergens
Yeon‐Jung Seo
Jonathan P. Mochel
Todd Atherly
Karin Allenspach
author_sort Aarti Kathrani
title Interleukin‐13 and interleukin‐33 mRNA are underexpressed in the duodenal mucosa of German Shepherd dogs with chronic enteropathy
title_short Interleukin‐13 and interleukin‐33 mRNA are underexpressed in the duodenal mucosa of German Shepherd dogs with chronic enteropathy
title_full Interleukin‐13 and interleukin‐33 mRNA are underexpressed in the duodenal mucosa of German Shepherd dogs with chronic enteropathy
title_fullStr Interleukin‐13 and interleukin‐33 mRNA are underexpressed in the duodenal mucosa of German Shepherd dogs with chronic enteropathy
title_full_unstemmed Interleukin‐13 and interleukin‐33 mRNA are underexpressed in the duodenal mucosa of German Shepherd dogs with chronic enteropathy
title_sort interleukin‐13 and interleukin‐33 mrna are underexpressed in the duodenal mucosa of german shepherd dogs with chronic enteropathy
publisher Wiley
series Journal of Veterinary Internal Medicine
issn 0891-6640
1939-1676
publishDate 2019-07-01
description Abstract Background A recent genome‐wide association study in German Shepherd dogs (GSDs) with chronic enteropathy (CE) has identified polymorphisms in the Th2 cytokine genes. Hypothesis/objective To determine if the expression of the Th2 cytokines, interleukin‐13 (IL‐13) and interleukin‐33 (IL‐33), is altered in the duodenal mucosa of GSDs with CE compared to non‐GSDs with CE and healthy dogs. Animals Twenty client‐owned dogs diagnosed with CE (10 GSDs and 10 non‐GSDs) at the Bristol Veterinary School and 8 healthy Beagle dogs from the Iowa State University Service Colony. Methods Retrospective study using archived paraffin‐embedded duodenal biopsy samples. A novel RNA in situ hybridization technology (RNAscope) was used to hybridize IL‐13 and IL‐33 mRNA probes onto at least 10 sections from duodenal biopsy samples for each dog. RNAscope signals were visualized using a microscope and semi‐quantitative assessment was performed by a single operator. Results Based on duodenal villus, subvillus, epithelial, and lamina propria average expression scores, GSDs with CE had significantly lower IL‐13 and IL‐33 mRNA expression compared to non‐GSDs with CE (IL‐13, P < .04; IL‐33, P < .02) and healthy Beagle dogs (IL‐13, P < .02; IL‐33, P < .004). Conclusions and Clinical Importance Similar to human patients with ulcerative colitis, a subtype of human inflammatory bowel disease, these data indicate that Th2 cytokines may be involved in the pathogenesis of CE in GSDs.
topic bowel
canine
cytokine
duodenum
inflammatory
Th2
url https://doi.org/10.1111/jvim.15544
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