4.6 Article

Conventional CD4+ T cells regulate IL-22-producing intestinal innate lymphoid cells

Journal

MUCOSAL IMMUNOLOGY
Volume 7, Issue 5, Pages 1045-1057

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/mi.2013.121

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Funding

  1. Penn-CHOP Joint Center for Digestive, Liver and Pancreatic Medicine [P30-DK050306]
  2. Penn Genome Frontiers Institute
  3. University of Pennsylvania Center for AIDS Research (CFAR) [P30 AI 045008, R01-AI57757]
  4. Training Program in Rheumatic Disease [5T32AR007442-25]

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The innate and adaptive immune systems in the intestine cooperate to maintain the integrity of the intestinal barrier and to regulate the composition of the resident microbiota. However, little is known about the crosstalk between the innate and adaptive immune systems that contribute to this homeostasis. We find that CD4 + Tcells regulate the number and function of barrier-protective innate lymphoid cells (ILCs), as well as production of antimicrobial peptides (AMPs), Reg3 gamma and Reg3 beta. RAG1 - / - mice lacking T and B cells had elevated ILC numbers, interleukin-22 (IL-22) production, and AMP expression, which were corrected by replacement of CD4 + Tcells. Major histocompatibility class II - / - (MHCII - / -) mice lacking CD4 + T cells also had increased ILCs, IL- 22, and AMPs, suggesting that negative regulation by CD4 + T cells occurs at steady state. We utilized transfers and genetically modified mice to show that reduction of IL- 22 is mediated by conventional CD4 + Tcells and is T- cell receptor dependent. The IL-22-AMP axis responds to commensal bacteria; however, neither the bacterial repertoire nor the gross localization of commensal bacteria differed between MHCII + / - and MHCII - / - littermates. These data define a novel ability of CD4 + T cells to regulate intestinal IL-22-producing ILCs and AMPs.

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