Intestinal epithelial glucocorticoid receptor promotes chronic inflammation–associated colorectal cancer
Shuang Tang, … , John A. Cidlowski, Xiaoling Li
Shuang Tang, … , John A. Cidlowski, Xiaoling Li
Published November 16, 2021
Citation Information: JCI Insight. 2021;6(24):e151815. https://doi.org/10.1172/jci.insight.151815.
View: Text | PDF
Research Article Gastroenterology Oncology

Intestinal epithelial glucocorticoid receptor promotes chronic inflammation–associated colorectal cancer

Abstract

Synthetic immunosuppressive glucocorticoids (GCs) are widely used to control inflammatory bowel disease (IBD). However, the impact of GC signaling on intestinal tumorigenesis remains controversial. Here, we report that intestinal epithelial GC receptor (GR), but not whole intestinal tissue GR, promoted chronic intestinal inflammation-associated colorectal cancer in both humans and mice. In patients with colorectal cancer, GR was enriched in intestinal epithelial cells and high epithelial cell GR levels were associated with poor prognosis. Consistently, intestinal epithelium–specific deletion of GR (GR iKO) in mice increased macrophage infiltration, improved tissue recovery, and enhanced antitumor response in a chronic inflammation–associated colorectal cancer model. Consequently, GR iKO mice developed fewer and less advanced tumors than control mice. Furthermore, oral GC administration in the early phase of tissue injury delayed recovery and accelerated the formation of aggressive colorectal cancers. Our study reveals that intestinal epithelial GR signaling repressed acute colitis but promoted chronic inflammation–associated colorectal cancer. Our study suggests that colorectal epithelial GR could serve as a predictive marker for colorectal cancer risk and prognosis. Our findings further suggest that, although synthetic GC treatment for IBD should be used with caution, there is a therapeutic window for GC therapy during colorectal cancer development in immunocompetent patients.

Authors

Shuang Tang, Zhan Zhang, Robert H. Oakley, Wenling Li, Weijing He, Xiaojiang Xu, Ming Ji, Qing Xu, Liang Chen, Alicia S. Wellman, Qingguo Li, Leping Li, Jian-Liang Li, Xinxiang Li, John A. Cidlowski, Xiaoling Li

×

Figure 7

Early-phase betamethasone treatment increases the growth of allografted colon carcinoma cells in mice.

Options: View larger image (or click on image) Download as PowerPoint
Early-phase betamethasone treatment increases the growth of allografted ...
(A and B) Early-phase oral BMZ treatment increases the growth of allografted CT26.WT carcinoma cells in BALB/c mice. Two-month-old immunocompetent BALB/c mice were treated and analyzed as described in the Methods. (A) Tumor volume was monitored, and (B) a final image of the dissected tumors as well as tumor weights are shown (n = 8–10; data represent mean ± SEM; *P < 0.05, Mann-Whitney test). (C and D) Early-phase oral BMZ treatment increases the growth of allografted CT26.WT colon carcinoma cells in NSG mice (n = 8–10, one outlier from each group was removed for tumor weight analysis using IQR analysis, in which any values outside the 1.5 × IQR range were considered outliers; data represent mean ± SEM; *P < 0.05, Mann-Whitney test). (E) The expression of macrophage markers, chemokines, and proliferation genes in allografted CT26.WT colon tumors. The allografted CT26.WT colon tumors in B and D were analyzed for the expression of the indicated genes by qPCR (n = 8–10; data represent mean ± SEM; *P < 0.05, **P < 0.01, ***P < 0.001, Mann-Whitney test). (F–I) Late-phase oral BMZ treatment increases the growth of allografted CT26.WT colon carcinoma cells in NSG mice but not BALB/c mice. Two-month-old immunocompetent BALB/c mice and NSG mice were allografted with CT26.WT cells, and tumor volume was monitored. When the average tumor size reached 30–40 mm3 (at day 16), mice in each strain were randomly divided into 2 groups and treated with vehicle or BMZ for the rest of the experiment (n = 8 tumors/group for both BALB/c mice and NSG mice; data represent mean ± SEM; *P < 0.05, Mann-Whitney test).