4.5 Article

Hyperactivated B cells in human inflammatory bowel disease

Journal

JOURNAL OF LEUKOCYTE BIOLOGY
Volume 86, Issue 4, Pages 1007-1016

Publisher

WILEY
DOI: 10.1189/jlb.0309203

Keywords

inflammation; Toll-like receptor 2; IL-8; Crohn's disease; ulcerative colitis

Funding

  1. Department of Medicine Pilot Award
  2. Boston University School of Medicine and the Evans Medical Foundation
  3. Broad Medical Research Program of The Broad Foundation
  4. BD Grant Award
  5. American Diabetes Association [DE018917]
  6. Smithwick Endowment Fund to the Department of Surgery

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IBD is characterized by a chronic, dysregulated immune response to intestinal bacteria. Past work has focused on the role of T cells and myeloid cells in mediating chronic gastrointestinal and systemic inflammation. Here, we show that circulating and tissue B cells from CD patients demonstrate elevated basal levels of activation. CD patient B cells express surface TLR2, spontaneously secrete high levels of IL-8, and contain increased ex vivo levels of phosphorylated signaling proteins. CD clinical activity correlates directly with B cell expression of IL-8 and TLR2, suggesting a positive relationship between these B cell inflammatory mediators and disease pathogenesis. In contrast, B cells from UC patients express TLR2 but generally do not demonstrate spontaneous IL-8 secretion; however, significant IL-8 production is inducible via TLR2 stimulation. Furthermore, UC clinical activity correlates inversely with levels of circulating TLR2 + B cells, which is opposite to the association observed in CD. In conclusion, TLR2 + B cells are associated with clinical measures of disease activity and differentially associated with CD-and UC-specific patterns of inflammatory mediators, suggesting a formerly unappreciated role of B cells in the pathogenesis of IBD J. Leukoc. Biol. 86: 1007-1016; 2009.

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