An innate cell-mediated, murine ulcerative colitis-like syndrome in the absence of nuclear factor of activated T cells.

6533b872fe1ef96bd12d3a6e

RESEARCH PRODUCT

An innate cell-mediated, murine ulcerative colitis-like syndrome in the absence of nuclear factor of activated T cells.

Laurie H. Glimcher Stanford L. Peng Ling Lin Andrea J. Gerth Markus F. Neurath

subject

T-Lymphocytes Biology Interleukin 21 Mice medicine Immune Tolerance Cytotoxic T cell Animals IL-2 receptor B-Lymphocytes Immunity Cellular Mice Inbred BALB C Hepatology NFATC Transcription Factors ZAP70 Innate lymphoid cell Gastroenterology Nuclear Proteins T helper cell Rectal Prolapse Natural killer T cell Acquired immune system Mice Mutant Strains DNA-Binding Proteins Mice Inbred C57BL medicine.anatomical_structure Immunology Cancer research Colitis Ulcerative Transcription Factors

description

Abstract Background & Aims: Nuclear factor of activated T cells transcription factors plays a central role in immunity by regulating the expression of multiple cytokines and other regulatory molecules, many of which have been heavily implicated in the pathogenesis of inflammatory bowel disease. However, few studies have directly investigated the nuclear factor of activated T cells proteins in inflammatory bowel disease. We describe here a specific role for nuclear factor of activated T cells c2 in the pathogenesis of murine inflammatory bowel disease. Methods: Mice deficient for nuclear factor of activated T cells c2, recombinase activating gene-2, or both and transgenic or nontransgenic for an anti-ovalbumin T-cell receptor or an anti-hen egg lysozyme B-cell receptor were studied. Adoptive transfers were performed of T or B cells or both from nuclear factor of activated T cells c2-deficient mice into nuclear factor of activated T cells c2-deficient recombinase activating gene-deficient animals, in the presence or absence of antibodies that neutralize interleukin-10 activity. Results: Nuclear factor of activated T cells c2-deficient, recombinase activating gene-deficient animals spontaneously developed a severe inflammatory bowel syndrome that resembled ulcerative colitis but was composed entirely of nonlymphocytes. The disease was suppressed by the adoptive transfer of polyclonal B-cell populations, even on neutralization of interleukin-10, but not by the presence of monoclonal T or B cells. Conclusions: Nuclear factor of activated T cells plays a critical role in the regulation of bowel inflammation by nonlymphoid immune cells, and B cells suppress bowel inflammation by innate immune cells. Such findings indicate a novel, interleukin-10-independent role for nuclear factor of activated T cells in the regulation of innate immunity and in intestinal immune tolerance.

year	journal	country	edition	language
2004-04-02	Gastroenterology

10.1053/j.gastro.2004.01.013 https://pubmed.ncbi.nlm.nih.gov/15057750