Epithelial TNF controls cell differentiation and CFTR activity to maintain intestinal mucin homeostasis
Efren A. Reyes, David Castillo-Azofeifa, Jérémie Rispal, Tomas Wald, Rachel K. Zwick, Brisa Palikuqi, Angela Mujukian, Shervin Rabizadeh, Alexander R. Gupta, James M. Gardner, Dario Boffelli, Zev J. Gartner, Ophir D. Klein
Efren A. Reyes, David Castillo-Azofeifa, Jérémie Rispal, Tomas Wald, Rachel K. Zwick, Brisa Palikuqi, Angela Mujukian, Shervin Rabizadeh, Alexander R. Gupta, James M. Gardner, Dario Boffelli, Zev J. Gartner, Ophir D. Klein
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Research Article Gastroenterology

Epithelial TNF controls cell differentiation and CFTR activity to maintain intestinal mucin homeostasis

Abstract

The gastrointestinal tract relies on the production, maturation, and transit of mucin to protect against pathogens and to lubricate the epithelial lining. Although the molecular and cellular mechanisms that regulate mucin production and movement are beginning to be understood, the upstream epithelial signals that contribute to mucin regulation remain unclear. Here, we report that the inflammatory cytokine tumor necrosis factor (TNF), generated by the epithelium, contributes to mucin homeostasis by regulating both cell differentiation and cystic fibrosis transmembrane conductance regulator (CFTR) activity. We used genetic mouse models and noninflamed samples from patients with inflammatory bowel disease (IBD) undergoing anti-TNF therapy to assess the effect of in vivo perturbation of TNF. We found that inhibition of epithelial TNF promotes the differentiation of secretory progenitor cells into mucus-producing goblet cells. Furthermore, TNF treatment and CFTR inhibition in intestinal organoids demonstrated that TNF promotes ion transport and luminal flow via CFTR. The absence of TNF led to slower gut transit times, which we propose results from increased mucus accumulation coupled with decreased luminal fluid pumping. These findings point to a TNF/CFTR signaling axis in the adult intestine and identify epithelial cell–derived TNF as an upstream regulator of mucin homeostasis.

Authors

Efren A. Reyes, David Castillo-Azofeifa, Jérémie Rispal, Tomas Wald, Rachel K. Zwick, Brisa Palikuqi, Angela Mujukian, Shervin Rabizadeh, Alexander R. Gupta, James M. Gardner, Dario Boffelli, Zev J. Gartner, Ophir D. Klein

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Figure 1

TNF and its receptors are expressed in defined spatial domains within epithelial crypts and villi.

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TNF and its receptors are expressed in defined spatial domains within ep...
(AC) RNAscope of Tnf, Tnfrsf1a (Tnfr1), and Tnfrsf1b (Tnfr2). (A) Tnf transcripts localize to the villus tip and the crypt base. (B) Tnfrsf1a transcripts are broadly expressed in the epithelium. (C) Tnfrsf1b transcripts are enriched in epithelial crypts compared with villi. White boxes highlight insets. Dashed lines outline the epithelium-mesenchyme border. (D) qPCR analysis of cells sorted by CD44 expression, CD44hi = crypt cells, CD44lo = villus cells. P values were calculated by unpaired multiple t test analysis with Welch’s correction (n = 6 mice per group). (EG) TNF, TNFR1, and TNFR2 immunofluorescence in control mice. (E) TNF is broadly present in the epithelium, with an enrichment in crypts. (F) TNFR1 is highly present in the top of the villus epithelium and gradually decreases toward the bottom of the crypt. (G) TNFR2 is enriched in crypts. Scale bars: 50 μm.