Epithelial Gab1 calibrates RIPK3-dependent necroptosis to prevent intestinal inflammation
Jiaqi Xu, Shihao Li, Wei Jin, Hui Zhou, Tingting Zhong, Xiaoqing Cheng, Yujuan Fu, Peng Xiao, Hongqiang Cheng, Di Wang, Yuehai Ke, Zhinong Jiang, Xue Zhang
Jiaqi Xu, Shihao Li, Wei Jin, Hui Zhou, Tingting Zhong, Xiaoqing Cheng, Yujuan Fu, Peng Xiao, Hongqiang Cheng, Di Wang, Yuehai Ke, Zhinong Jiang, Xue Zhang
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Research Article Gastroenterology Inflammation

Epithelial Gab1 calibrates RIPK3-dependent necroptosis to prevent intestinal inflammation

Abstract

As a hallmark of inflammatory bowel disease (IBD), elevated intestinal epithelial cell (IEC) death compromises the gut barrier, activating the inflammatory response and triggering more IEC death. However, the precise intracellular machinery that prevents IEC death and breaks this vicious feedback cycle remains largely unknown. Here, we report that Grb2-associated binder 1 (Gab1) expression is decreased in patients with IBD and inversely correlated with IBD severity. Gab1 deficiency in IECs accounted for the exacerbated colitis induced by dextran sodium sulfate owing to sensitizing IECs to receptor-interaction protein kinase 3–mediated (RIPK3-mediated) necroptosis, which irreversibly disrupted the homeostasis of the epithelial barrier and promoted intestinal inflammation. Mechanistically, Gab1 negatively regulated necroptosis signaling through inhibiting the formation of RIPK1/RIPK3 complex in response to TNF-α. Importantly, administration of RIPK3 inhibitor revealed a curative effect in epithelial Gab1-deficient mice. Further analysis indicated mice with Gab1 deletion were prone to inflammation-associated colorectal tumorigenesis. Collectively, our study defines a protective role for Gab1 in colitis and colitis-driven colorectal cancer by negatively regulating RIPK3-dependent necroptosis, which may serve as an important target to address necroptosis and intestinal inflammation–related disease.

Authors

Jiaqi Xu, Shihao Li, Wei Jin, Hui Zhou, Tingting Zhong, Xiaoqing Cheng, Yujuan Fu, Peng Xiao, Hongqiang Cheng, Di Wang, Yuehai Ke, Zhinong Jiang, Xue Zhang

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Figure 8

Selective RIPK3 inhibitor GSK’872 rescues epithelial Gab1-deficient mice from DSS-induced colitis.

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Selective RIPK3 inhibitor GSK’872 rescues epithelial Gab1-deficient mice...
Gab1fl/fl and Gab1IEC-KO mice were exposed to 3% DSS in drinking water as previously described, then intraperitoneally (i.p.) treated with either the vehicle control or GSK’872 at a dose of 10 mg/kg body weight once daily throughout the entire experimental period. n = 4, 5, 8, 8, for Gab1fl/fl + DSS + control group, Gab1IEC-KO +DSS + control group, Gab1fl/fl + DSS+ GSK’872 group, Gab1IEC-KO + DSS + GSK’872 group, respectively. (A) Relative percentage change in body weight, as well as diarrhea and rectal bleeding scores, were assessed daily. (B) Gross morphology images of the colon from Gab1fl/fl and Gab1IEC-KO mice with different treatment. The colon lengths were measured on day 7. (C) Representative H&E-stained images and histological scores of the distal colon were assessed on day 7. Scale bars, 100 μm. (D) Representative PAS staining of colon sections from mice sacrificed at day 7. Scale bars, 100 μm. (E) Representative images of TUNEL staining (green or gray) of colonic sections on day 7. Scale bars, 100 μm (overview) and 50 μm (magnification). (F) Immunoblotting of colonic protein from the DSS-challenged mice with or without GSK’872 administration on day 7. Quantitative data were presented as the mean ± SEM. Statistical analysis was performed by 2-way ANOVA with multiple comparisons test; *P < 0.05.