Sensitization to and Challenge with Gliadin Induce Pancreatitis and Extrapancreatic Inflammation in HLA-DQ8 Mice: An Animal Model of Type 1 Autoimmune Pancreatitis.

Sung Hoon MOON; Jihun KIM; Mi Young KIM; Do Hyun PARK; Tae Jun SONG; Sun A KIM; Sang Soo LEE; Dong Wan SEO; Sung Koo LEE; Myung Hwan KIM

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Sensitization to and Challenge with Gliadin Induce Pancreatitis and Extrapancreatic Inflammation in HLA-DQ8 Mice: An Animal Model of Type 1 Autoimmune Pancreatitis.

Author: Sung Hoon MOON ¹ ; Jihun KIM ; Mi Young KIM ; Do Hyun PARK ; Tae Jun SONG ; Sun A KIM ; Sang Soo LEE ; Dong Wan SEO ; Sung Koo LEE ; Myung Hwan KIM
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1. Department of Internal Medicine, Hallym University Sacred Heart Hospital, Hallym University College of Medicine, Anyang, Korea.
Publication Type:Original Article
Keywords: Autoimmune diseases; Pancreatitis; Celiac disease
MeSH: Animals; Animals*; Atrophy; Autoimmune Diseases; Bile Ducts; Celiac Disease; Ceruletide; Eating; Edible Grain; Fibrosis; Gliadin*; Humans; Inflammation*; Kidney; Leukocytes; Lung; Mice*; Mice, Transgenic; Models, Animal*; Pancreatitis*; Plasma Cells; Salivary Glands
From:Gut and Liver 2016;10(5):842-850
CountryRepublic of Korea
Language:English
Abstract: BACKGROUND/AIMS: The aim of this study was to establish a pathogenetic mechanism of pancreatitis in celiac disease and IgG4-related disease using gluten-sensitive human leukocyte antigen (HLA)-DQ8 transgenic mice. METHODS: Transgenic mice expressing HLA-DQ8 genes were utilized. Control mice were not sensitized but were fed gliadin-free rice cereal. Experimental groups consisted of gliadin-sensitized and gliadin-challenged mice; nonsensitized mice with cerulein hyperstimulation; and gliadin-sensitized and gliadin-challenged mice with cerulein hyperstimulation. RESULTS: Gliadin-sensitized and gliadin-challenged mice with cerulein hyperstimulation showed significant inflammatory cell infiltrates, fibrosis and acinar atrophy compared with the control mice and the other experimental groups. The immunohistochemical analysis showed greater IgG1-positive plasma cells in the inflammatory infiltrates of gliadin-sensitized and gliadin-challenged mice with cerulein hyperstimulation compared with the control mice and the other experimental groups. Gliadin-sensitized and gliadin-challenged mice with cerulein hyperstimulation or gliadin-sensitized and gliadin-challenged mice showed IgG1-stained inflammatory cell infiltrates in the extrapancreatic organs, including the bile ducts, salivary glands, kidneys, and lungs. CONCLUSIONS: Gliadin-sensitization and cerulein hyperstimulation of gluten-sensitive HLA-DQ8 transgenic mice resulted in pancreatitis and extrapancreatic inflammation. This animal model suggests that chronic gliadin ingestion in a susceptible individual with the HLA-DQ8 molecule may be associated with pancreatitis and extrapancreatic inflammation.