Abstract

Despite decades of research, the basic pathogenetic mechanisms involved in inflammatory bowel disease (IBD) remain elusive, but the answers appear to lie in the scientific fields of immunology and genetics and these are the major areas addressed in this proposal. The basic theme of this Program Project relates to the immunologic mechanisms determining chronic inflammation in the intestine, the impact of chronic enteritis on the mucosal immune system, the mechanism of antigen handling in the intact and inflamed colon, and the genetic influences that determine susceptibility to disease, as well as the interplay and interaction among these areas. The focus of these studies will be on newly developed mouse models of colitis including spontaneous colitis in C3H/HeJBir mice, a substrain which was generated during the initial phase of this project. Although no model exactly duplicates human IBD, models can allow important insights into certain disease mechanisms. The mouse has been chosen because of the rich array of techniques and reagents available only in this species in both immunology and genetics. The Program Project will consist of four Projects and two Cores. Project #1, will focus on the enteric bacterial antigens recognized by the immune system during chronic colitis, particularly by T cells, the role that such T cells play in disease pathogenesis, and how such T cells are regulated. Project #2 will study a number of issues of mucosal immunity, oral tolerance, and isotype regulation in the setting of chronic intestinal inflammation. Project #3 will exploit two powerful new technologies, a T cell transgenic mouse, and in situ hybridization techniques, to examine antigen handling and T cell induction in the normal and inflamed colon. Project #4 will be located at the Jackson Laboratory in Bar Harbor, ME. This project will map genes important in susceptibility to colitis induction in inbred mouse strains, including the G3H/HeJBir colitic substrain. These projects will be supported by an Administrative Core which will provide administrative and fiscal support and coordination, and an Animal Model Core which will centralize the production of mice with experimental colitis, maintain strict quality control, and provide a centralized pathologic analysis. These studies should generate new concepts and paradigms to test in man, and possibly new approaches to immunotherapy, as has happened with mouse models of other diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Program Projects (P01)
Project #
2P01DK044240-04
Application #
2143654
Study Section
Diabetes, Endocrinology and Metabolic Diseases B Subcommittee (DDK)
Project Start
1991-09-01
Project End
1999-08-31
Budget Start
1994-09-15
Budget End
1995-08-31
Support Year
4
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
University of Alabama Birmingham
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
004514360
City
Birmingham
State
AL
Country
United States
Zip Code
35294

  Publications

Jurisic, Giorgia; Sundberg, John P; Detmar, Michael (2013) Blockade of VEGF receptor-3 aggravates inflammatory bowel disease and lymphatic vessel enlargement. Inflamm Bowel Dis 19:1983-9
Luckey, C John; Weaver, Casey T (2012) Stem-cell-like qualities of immune memory; CD4+ T cells join the party. Cell Stem Cell 10:107-8
Jurisic, G; Sundberg, J P; Bleich, A et al. (2010) Quantitative lymphatic vessel trait analysis suggests Vcam1 as candidate modifier gene of inflammatory bowel disease. Genes Immun 11:219-31
Bleich, Andre; Büchler, Gwen; Beckwith, Jason et al. (2010) Cdcs1 a major colitis susceptibility locus in mice; subcongenic analysis reveals genetic complexity. Inflamm Bowel Dis 16:765-75
Maynard, Craig L; Weaver, Casey T (2008) Diversity in the contribution of interleukin-10 to T-cell-mediated immune regulation. Immunol Rev 226:219-33
Elson, Charles O; Cong, Yingzi; Weaver, Casey T et al. (2007) Monoclonal anti-interleukin 23 reverses active colitis in a T cell-mediated model in mice. Gastroenterology 132:2359-70
Duverger, Alexandra; Jackson, Raymond J; van Ginkel, Frederick W et al. (2006) Bacillus anthracis edema toxin acts as an adjuvant for mucosal immune responses to nasally administered vaccine antigens. J Immunol 176:1776-83
Elson, Charles O; Cong, Yingzi; Qi, Fengxia et al. (2006) Molecular approaches to the role of the microbiota in inflammatory bowel disease. Ann N Y Acad Sci 1072:39-51
Konrad, Astrid; Cong, Yingzi; Duck, Wayne et al. (2006) Tight mucosal compartmentation of the murine immune response to antigens of the enteric microbiota. Gastroenterology 130:2050-9
van Ginkel, Frederik W; Jackson, Raymond J; Yoshino, Naoto et al. (2005) Enterotoxin-based mucosal adjuvants alter antigen trafficking and induce inflammatory responses in the nasal tract. Infect Immun 73:6892-902

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