Abstract
Annual Review of Immunology
Vol. 20:
495-549
(Volume publication date April 2002)
(doi:10.1146/annurev.immunol.20.100301.064816)
T HE I MMUNOLOGY OF M UCOSAL M ODELS OF I NFLAMMATION1Warren Strober,1 Ivan J. Fuss,1 and Richard S. Blumberg21Mucosal Immunity Section, Laboratory of Clinical Investigation, NIAID, NIH, Bethesda, Maryland 20892-1890; e-mail: wstrober@niaid.nih.gov 2Division of Gastroenterology, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts 02115 ▪ Abstract In recent years the status of the inflammatory bowel diseases (IBDs) as canonical autoimmune diseases has risen steadily with the recognition that these diseases are, at their crux, abnormalities in mucosal responses to normally harmless antigens in the mucosal microflora and therefore responses to antigens that by their proximity and persistence are equivalent to self-antigens. This new paradigm is in no small measure traceable to the advent of multiple models of mucosal inflammation whose very existence is indicative of the fact that many types of immune imbalance can lead to loss of tolerance for mucosal antigens and thus inflammation centered in the gastrointestinal tract. We analyze the immunology of the IBDs through the lens of the murine models, first by drawing attention to their common features and then by considering individual models at a level of detail necessary to reveal their individual capacities to provide insight into IBD pathogenesis. What emerges is that murine models of mucosal inflammation have given us a road map that allows us to begin to define the immunology of the IBDs in all its complexity and to find unexpected ways to treat these diseases. Most recent citing papers (via CrossRef)3,3′-diindolylmethane attenuates colonic inflammation and tumorigenesis in mice Inflammatory Bowel Diseases 15(8):1164-1173 (2009) Homeostatic (IL-7) and effector (IL-17) cytokines as distinct but complementary target for an optimal therapeutic strategy in inflammatory bowel disease Current Opinion in Gastroenterology 25(4):306-313 (2009) A probiotic strain of
Escherichia coli
, Nissle 1917, given orally exerts local and systemic anti-inflammatory effects in lipopolysaccharide-induced sepsis in mice British Journal of Pharmacology (2009) Persistent retention of colitogenic CD4
+
memory T cells causes inflammatory bowel diseases to become intractable Inflammatory Bowel Diseases 15(6):926-934 (2009) Crohn’s Disease: an Immune Deficiency State Clinical Reviews in Allergy & Immunology (2009)
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