Goblet cells deliver luminal antigen to CD103^sup +^ dendritic cells in the small intestine

The intestinal immune system is exposed to a mixture of foreign antigens from diet, commensal flora and potential pathogens. Understanding how pathogen-specific immunity is elicited while avoiding inappropriate responses to the background of innocuous antigens is essential for understanding and trea...

Full description

Saved in:
Bibliographic Details
Published inNature (London) Vol. 483; no. 7389; p. 345
Main Authors McDole, Jeremiah R, Wheeler, Leroy W, McDonald, Keely G, Wang, Baomei, Konjufca, Vjollca, Knoop, Kathryn A, Newberry, Rodney D, Miller, Mark J
Format Journal Article
LanguageEnglish
Published London Nature Publishing Group 15.03.2012
Subjects
Proteins
Rodents
Small intestine
Studies
Online AccessGet full text

Cover

More Information
Summary:The intestinal immune system is exposed to a mixture of foreign antigens from diet, commensal flora and potential pathogens. Understanding how pathogen-specific immunity is elicited while avoiding inappropriate responses to the background of innocuous antigens is essential for understanding and treating intestinal infections and inflammatory diseases. The ingestion of protein antigen can induce oral tolerance, which is mediated in part by a subset of intestinal dendritic cells (DCs) that promote the development of regulatory T cells. The lamina propria (LP) underlies the expansive single-cell absorptive villous epithelium and contains a large population of DCs (CD11c^sup +^ CD11b^sup +^ MHCII^sup +^ cells) comprised of two predominant subsets: CD103^sup +^ CX^sub 3^CR1^sup -^ DCs, which promote IgA production, imprint gut homing on lymphocytes and induce the development of regulatory T cells, and CD103^sup -^ CX^sub 3^CR1^sup +^ DCs (with features of macrophages), which promote tumour necrosis factor-α (TNF-α) production, colitis, and the development of T^sub H^17 T cells. However, the mechanisms by which different intestinal LP-DC subsets capture luminal antigens in vivo remains largely unexplored. Using a minimally disruptive in vivo imaging approach we show that in the steady state, small intestine goblet cells (GCs) function as passages delivering low molecular weight soluble antigens from the intestinal lumen to underlying CD103^sup +^ LP-DCs. The preferential delivery of antigens to DCs with tolerogenic properties implies a key role for this GC function in intestinal immune homeostasis. [PUBLICATION ABSTRACT]
ISSN:0028-0836
1476-4687