TSLP/dendritic cell axis promotes CD4+ T cell tolerance to the gut microbiome
Jonathan L. Messerschmidt, … , Kaitlin E. Dempsey, Shadmehr Demehri
Jonathan L. Messerschmidt, … , Kaitlin E. Dempsey, Shadmehr Demehri
Published July 10, 2023
Citation Information: JCI Insight. 2023;8(13):e160690. https://doi.org/10.1172/jci.insight.160690.
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Research Article Gastroenterology Immunology

TSLP/dendritic cell axis promotes CD4+ T cell tolerance to the gut microbiome

Abstract

Thymic stromal lymphopoietin (TSLP) overexpression is widely associated with atopy. However, TSLP is expressed in normal barrier organs, suggesting a homeostatic function. To determine the function of TSLP in barrier sites, we investigated the impact of endogenous TSLP signaling on the homeostatic expansion of CD4+ T cells in adult mice. Surprisingly, incoming CD4+ T cells induced lethal colitis in adult Rag1-knockout animals that lacked the TSLP receptor (Rag1KOTslprKO). Endogenous TSLP signaling was required for reduced CD4+ T cell proliferation, Treg differentiation, and homeostatic cytokine production. CD4+ T cell expansion in Rag1KOTslprKO mice was dependent on the gut microbiome. The lethal colitis was rescued by parabiosis between Rag1KOTslprKO and Rag1KO animals and wild-type dendritic cells (DCs) suppressed CD4+ T cell–induced colitis in Rag1KOTslprKO mice. A compromised T cell tolerance was noted in TslprKO adult colon, which was exacerbated by anti–PD-1 and anti–CTLA-4 therapy. These results reveal a critical peripheral tolerance axis between TSLP and DCs in the colon that blocks CD4+ T cell activation against the commensal gut microbiome.

Authors

Jonathan L. Messerschmidt, Marjan Azin, Kaitlin E. Dempsey, Shadmehr Demehri

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Figure 7

TSLP signaling protects the colon from immune checkpoint blockade–induced colitis.

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TSLP signaling protects the colon from immune checkpoint blockade–induce...
(A) Representative colon H&E staining of TslprKO and WT mice treated intraperitoneally with 200 μg of anti–CTLA-4/anti–PD-1 immune checkpoint blockade (ICB) therapy every 3 days for 15 days and harvested on day 15 after therapy. Insets highlight the increased lymphocytic infiltrate in the TslprKO compared with WT colon. Scale bars: 50 μm. (B) Colitis scoring of TslprKO (n = 6) and WT (n = 6) on day 15 after therapy. Fisher’s exact test. (C and D) Representative CD3/CD4 (C) and CD3/CD8 staining (D) of TslprKO and WT colon 15 days after ICB treatment. CD3 single-positive cells are highlighted with arrows and double-positive cells are highlighted with arrowheads. Note the increased mucosal CD4+ T cell presence preferentially in TslprKO compared with WT colon. Scale bar: 50 μm. (EG) CD3+ T (E), CD4+ T (F), and CD8+ T cell (G) count in TslprKO (n = 5) and WT (n = 5) colon on day 15 after ICB therapy. CD3+, CD3+CD4+, and CD3+CD8+ mucosal T cells were quantified in 10 randomly selected HPFs per colon at the end of the study. Each dot represents 1 HPF; bar graphs show mean + SD. ****P < 0.0001 by unpaired, 2-tailed t test. NS, not significant.