Lin, Jieru Egeria, Snook, Adam Eugene, Li, Peng, Stoecker, Brian Arthur, Kim, Gilbert Won, Magee, Michael Sullivan, Mejia Garcia, Alex Vladimir, Valentino, Michael Anthony, Hyslop, Terry, Schulz, Stephanie, Waldman, Scott Arthur, Lin, Jieru Egeria, Snook, Adam Eugene, Li, Peng, Stoecker, Brian Arthur, Kim, Gilbert Won, Magee, Michael Sullivan, Mejia Garcia, Alex Vladimir, Valentino, Michael Anthony, Hyslop, Terry, Schulz, Stephanie, and Waldman, Scott Arthur
The barrier separating mucosal and systemic compartments comprises epithelial cells, annealed by tight junctions, limiting permeability. GUCY2C recently emerged as an intestinal tumor suppressor coordinating AKT1-dependent crypt-villus homeostasis. Here, the contribution of GUCY2C to barrier integrity opposing colitis and systemic tumorigenesis is defined. Mice deficient in GUCY2C (Gucy2c−/−) exhibited barrier hyperpermeability associated with reduced junctional proteins. Conversely, activation of GUCY2C in mice reduced barrier permeability associated with increased junctional proteins. Further, silencing GUCY2C exacerbated, while activation reduced, chemical barrier disruption and colitis. Moreover, eliminating GUCY2C amplified, while activation reduced, systemic oxidative DNA damage. This genotoxicity was associated with increased spontaneous and carcinogen-induced systemic tumorigenesis in Gucy2c−/− mice. GUCY2C regulated barrier integrity by repressing AKT1, associated with increased junction proteins occludin and claudin 4 in mice and Caco2 cells in vitro. Thus, GUCY2C defends the intestinal barrier, opposing colitis and systemic genotoxicity and tumorigenesis. The therapeutic potential of this observation is underscored by the emerging clinical development of oral GUCY2C ligands, which can be used for chemoprophylaxis in inflammatory bowel disease and cancer.