4.5 Article

Crohn's Disease Patients Uniquely Contain Inflammatory Responses to Flagellin in a CD4 Effector Memory Subset

期刊

INFLAMMATORY BOWEL DISEASES
卷 28, 期 12, 页码 1893-1903

出版社

OXFORD UNIV PRESS INC
DOI: 10.1093/ibd/izac146

关键词

effector memory CD4 T cells; cytokines; flagellin antigen; barrier dysfunction

资金

  1. Department of Veterans Affairs [CX0001530]
  2. University of Nebraska Medical Center

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Crohn's disease patients exhibit inflammatory cytokine responses to flagellin antigens in an expanded effector memory CD4 subset that is not present in ulcerative colitis or non-inflammatory bowel disease control subjects. These cells are correlated with levels of specific anti-flagellin antibodies.
Background Specific microbial antigens stimulate production of antibodies indicative of the aberrant immune response in Crohn's disease (CD). We tested for T cell reactivity linkage to B cell responses and now report on the prevalence, functionality, and phenotypic differences of flagellin-specific T cells among CD patients, ulcerative colitis (UC) patients, and control subjects and association with clinical features and flagellin seropositivity within CD patients. Methods Sera from non-inflammatory bowel disease control subjects, CD patients, and UC patients were probed for antibody reactivity to gut bacterial recombinant flagellin antigens. Peripheral blood mononuclear cells were measured for flagellin antigen (CBir1, A4 Fla2, FlaX) or control (Candida albicans, and CytoStim) reactivity analyzed by flow cytometry for CD154 and cytokine expression on CD4(+) T cells. Supernatants from post-flagellin-stimulated and unstimulated cells were used to measure effects on epithelial barrier function. Results CD patients had a significantly higher percentage of flagellin-specific CD154(+) CD4(+) cells that have an effector memory T helper 1 and T helper 17 phenotype compared with UC patients and healthy control subjects. There was a positive correlation between the frequency of flagellin-specific CD154(+) CD4(+) effector memory T cells and serum levels of anti-flagellin immunoglobulin G in the CD patients. In addition, A4 Fla2-reactive T cells from active CD patients produced cytokines that can decrease barrier function in a gut epithelium. Conclusions These findings demonstrate a Crohn's-associated flagellin-reactive CD4 cell subset distinct from UC patients and control subjects. There is a link between these cells and flagellin seropositivity. This CD4 cell subset could reflect a particular endophenotype of CD, leading to novel insight into its pathology and treatment. Lay Summary Crohn's disease patients display inflammatory cytokine responses to flagellin antigens in an expanded effector memory CD4 subset that is not seen in ulcerative colitis or non-inflammatory bowel disease control subjects. These cells correlate with levels of the specific cognate anti-flagellin antibodies.

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