Loss of gastrokine-2 drives premalignant gastric inflammation and tumor progression
Trevelyan R. Menheniott, … , Louise M. Judd, Andrew S. Giraud
Trevelyan R. Menheniott, … , Louise M. Judd, Andrew S. Giraud
Published March 14, 2016
Citation Information: J Clin Invest. 2016;126(4):1383-1400. https://doi.org/10.1172/JCI82655.
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Research Article Oncology

Loss of gastrokine-2 drives premalignant gastric inflammation and tumor progression

Abstract

Chronic mucosal inflammation is associated with a greater risk of gastric cancer (GC) and, therefore, requires tight control by suppressive counter mechanisms. Gastrokine-2 (GKN2) belongs to a family of secreted proteins expressed within normal gastric mucosal cells. GKN2 expression is frequently lost during GC progression, suggesting an inhibitory role; however, a causal link remains unsubstantiated. Here, we developed Gkn2 knockout and transgenic overexpressing mice to investigate the functional impact of GKN2 loss in GC pathogenesis. In mouse models of GC, decreased GKN2 expression correlated with gastric pathology that paralleled human GC progression. At baseline, Gkn2 knockout mice exhibited defective gastric epithelial differentiation but not malignant progression. Conversely, Gkn2 knockout in the IL-11/STAT3-dependent gp130F/F GC model caused tumorigenesis of the proximal stomach. Additionally, gastric immunopathology was accelerated in Helicobacter pylori–infected Gkn2 knockout mice and was associated with augmented T helper cell type 1 (Th1) but not Th17 immunity. Heightened Th1 responses in Gkn2 knockout mice were linked to deregulated mucosal innate immunity and impaired myeloid-derived suppressor cell activation. Finally, transgenic overexpression of human gastrokines (GKNs) attenuated gastric tumor growth in gp130F/F mice. Together, these results reveal an antiinflammatory role for GKN2, provide in vivo evidence that links GKN2 loss to GC pathogenesis, and suggest GKN restoration as a strategy to restrain GC progression.

Authors

Trevelyan R. Menheniott, Louise O’Connor, Yok Teng Chionh, Jan Däbritz, Michelle Scurr, Benjamin N. Rollo, Garrett Z. Ng, Shelley Jacobs, Angelique Catubig, Bayzar Kurklu, Stephen Mercer, Toshinari Minamoto, David E. Ong, Richard L. Ferrero, James G. Fox, Timothy C. Wang, Philip Sutton, Louise M. Judd, Andrew S. Giraud

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Figure 4

Cellular and molecular analysis of gastric epithelial differentiation in Gkn2–/– mice.

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Cellular and molecular analysis of gastric epithelial differentiation in...
(A) Expression of gastric trefoil factor and mucin genes in 12-week-old Gkn2–/– (n = 11) and WT (n = 8) corpus by QRT-PCR. (B) Characterization of SMC differentiation in 12-week-old WT and Gkn2–/– corpus and Gkn2–/– lesion mucosa by AB-PAS staining (top row) and immunofluorescent staining for MUC5AC and TFF1 proteins (bottom row). Scale bar: 20 μm. (C) Immunofluorescent quantitation of MNCs (MNC, GSII); parietal cells (PC, HK ATPase-β); and zymogenic cells (ZC, pepsinogen II) in 12-week-old WT and Gkn2–/– corpus mucosa (n = 6 per group). Scale bar: 20 μm. (D) Gastric acidity determined by pH measurement of stomach contents in Gkn2–/– (n = 11) and WT (n = 8) mice. (E) QRT-PCR analysis of gastrin mRNA expression in antral stomachs of Gkn2–/– (n = 11) and WT (n = 8) mice. Error bars represent mean ± SEM. P values were determined using a 2-tailed Student’s t test: *P < 0.05; **P < 0.01; ***P < 0.001.