SMAD4 TGF-β–independent function preconditions naive CD8+ T cells to prevent severe chronic intestinal inflammation
Ramdane Igalouzene, … , Julien C. Marie, Saïdi M’Homa Soudja
Ramdane Igalouzene, … , Julien C. Marie, Saïdi M’Homa Soudja
Published April 15, 2022
Citation Information: J Clin Invest. 2022;132(8):e151020. https://doi.org/10.1172/JCI151020.
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Research Article Gastroenterology Immunology

SMAD4 TGF-β–independent function preconditions naive CD8+ T cells to prevent severe chronic intestinal inflammation

Abstract

SMAD4, a mediator of TGF-β signaling, plays an important role in T cells to prevent inflammatory bowel disease (IBD). However, the precise mechanisms underlying this control remain elusive. Using both genetic and epigenetic approaches, we revealed an unexpected mechanism by which SMAD4 prevents naive CD8+ T cells from becoming pathogenic for the gut. Prior to the engagement of the TGF-β receptor, SMAD4 restrains the epigenetic, transcriptional, and functional landscape of the TGF-β signature in naive CD8+ T cells. Mechanistically, prior to TGF-β signaling, SMAD4 binds to promoters and enhancers of several TGF-β target genes, and by regulating histone deacetylation, suppresses their expression. Consequently, regardless of a TGF-β signal, SMAD4 limits the expression of TGF-β negative feedback loop genes, such as Smad7 and Ski, and likely conditions CD8+ T cells for the immunoregulatory effects of TGF-β. In addition, SMAD4 ablation conferred naive CD8+ T cells with both a superior survival capacity, by enhancing their response to IL-7, as well as an enhanced capacity to be retained within the intestinal epithelium, by promoting the expression of Itgae, which encodes the integrin CD103. Accumulation, epithelial retention, and escape from TGF-β control elicited chronic microbiota-driven CD8+ T cell activation in the gut. Hence, in a TGF-β–independent manner, SMAD4 imprints a program that preconditions naive CD8+ T cell fate, preventing IBD.

Authors

Ramdane Igalouzene, Hector Hernandez-Vargas, Nicolas Benech, Alexandre Guyennon, David Bauché, Célia Barrachina, Emeric Dubois, Julien C. Marie, Saïdi M’Homa Soudja

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Figure 9

The TGF-β–independent function of SMAD4 that restrains CD103 and IL-7R occurs in CD8+ T cells at the naive stage.

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The TGF-β–independent function of SMAD4 that restrains CD103 and IL-7R o...
(A) Experimental procedure for TAT-CRE experiment. Naive and memory CD8+ T cells were purified from either Smad4fl/fl Stopfl/fl Rosa26EYFP or Smad4wt/wt Stopfl/fl Rosa26EYFP mice and treated with TAT-CRE recombinant protein prior to transfer into RAG2-KO mice and 3 weeks later, cells were recovered and analyzed by flow cytometry. (B) Histograms illustrating the expression of CD103 and CD127 in YFP+ (recombined) in the naive (n = 7) or memory state (n = 6) CD8+ T cells and YFP (nonrecombined) counterpart CD8+ T cells from Smad4fl/fl Stopfl/fl Rosa26EYFP mice. (C) Similarly, histograms depicting the expression of CD103 and CD127 in YFP+ in the naive (n = 7) or memory state (n = 4) CD8+ T cells and YFP counterpart CD8+ T cells from Smad4wt/wt Stopfl/fl Rosa26EYFP mice. The data in panels B and C are expressed as percentage or MFI. Each symbol represents an individual mouse and n = 4 or more for each group. All data represent at least 3 independent experiments and are presented as mean ± SD. Data were analyzed by a paired Student’s t test. **P < 0.01, ***P < 0.001. NS, not significant (P > 0.05).