Retinoic acid induces homing of protective T and B cells to the gut after subcutaneous immunization in mice
Swantje I. Hammerschmidt, … , Oliver Pabst, Reinhold Förster
Swantje I. Hammerschmidt, … , Oliver Pabst, Reinhold Förster
Published July 1, 2011
Citation Information: J Clin Invest. 2011;121(8):3051-3061. https://doi.org/10.1172/JCI44262.
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Research Article

Retinoic acid induces homing of protective T and B cells to the gut after subcutaneous immunization in mice

Abstract

Diarrheal diseases represent a major health burden in developing countries. Parenteral immunization typically does not induce efficient protection against enteropathogens because it does not stimulate migration of immune cells to the gut. Retinoic acid (RA) is critical for gut immunity, inducing upregulation of gut-homing receptors on activated T cells. In this study, we have demonstrated that RA can redirect immune responses elicited by s.c. vaccination of mice from skin-draining inguinal LNs (ingLNs) to the gut. When present during priming, RA induced robust upregulation of gut-homing receptors in ingLNs, imprinting gut-homing capacity on T cells. Concurrently, RA triggered the generation of gut-tropic IgA+ plasma cells in ingLNs and raised the levels of antigen-specific IgA in the intestinal lumen and blood. RA applied s.c. in vivo induced autonomous RA production in ingLN DCs, further driving efficient induction of gut-homing molecules on effector cells. Importantly, RA-supplemented s.c. immunization elicited a potent immune response in the small intestine that protected mice from cholera toxin–induced diarrhea and diminished bacterial loads in Peyer patches after oral infection with Salmonella. Thus, the use of RA as a gut-homing navigator represents a powerful tool to induce protective immunity in the intestine after s.c. immunization, offering what we believe to be a novel approach for vaccination against enteropathogens.

Authors

Swantje I. Hammerschmidt, Michaela Friedrichsen, Jasmin Boelter, Marcin Lyszkiewicz, Elisabeth Kremmer, Oliver Pabst, Reinhold Förster

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Figure 4

Skin-draining ingLNs of RA-treated mice support induction of gut-homing receptor and IgA expression on B cells.

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Skin-draining ingLNs of RA-treated mice support induction of gut-homing ...
Mice were immunized on days 0 and 10 either s.c. with 1 μg CT or orally with 10 μg CT. A group of s.c. immunized mice additionally received s.c. RA injections on days 0, 1, 2, 3, 6, 10, and 13 after antigen delivery. On day 14, mice were sacrificed. (A) Levels of CT-specific Ig in serum and intestinal wash were determined by ELISA. Results are pooled from 4 independent experiments with at least 9 mice total per group. (B) Number of anti-CT IgA-secreting cells in the small intestinal lamina propria (LP), assessed by ELISPOT. Bars denote mean values; symbols denote individual mice pooled from 4 independent experiments. (CH) Sections from ingLNs of s.c. immunized mice with (D and E) or without (C and F) RA treatment were either analyzed at day 14 by fluorescence microscopy for IgA and Lyve-1 (C and D) or stained for IgA, CCR9, and IgD (E and F). Sections from ingLNs (G) and mLNs (H) from RA-treated s.c. immunized mice were stained for IgA and CT-binding cells. Images are representative for 6 mice analyzed per group in 2 independent experiments. Scale bars: 200 μm (C and D); 50 μm (E and F); 25 μm (G and H). *P < 0.05; **P < 0.01; ***P < 0.001.