Abstract: | Background—Transforminggrowth factor α (TGF-α) knockout mice have increased susceptibilityto dextran sodium sulphate (DSS) induced colitis. Aim—To substantiatethe findings that TGF-α is a key mediator of colonic mucosalprotection and/or repair mechanisms by evaluating the susceptibility ofmice overexpressing TGF-α to DSS induced colitis. Methods—TGF-αoverexpression was induced in transgenic mice by ZnSO4administration in drinking water (TG+). Three groups were used ascontrols: one transgenic group without ZnSO4 administration (TG−), and two non-transgenic littermate groups receivingZnSO4 (Non-TG+) or only water (Non-TG−). Acute colitiswas induced in all groups by administration of DSS (5%, w/v) indrinking water for six days ad libitum. Results—About 35-39%of the entire colonic mucosa was destroyed in Non-TG−, Non-TG+, andTG− animals compared with 9% in TG+ mice. The crypt damage score was18.7 (0.9), 18.2 (1.0), 18.9(0.8), and 6.8 (1.5) (means (SEM)) inNon-TG−, Non-TG+, TG−, and TG+ mice respectively. Mucin andbromodeoxyuridine staining were markedly enhanced in colons of TG+ micecompared with controls, indicating increased mucosal protection and regeneration. Conclusions—Thesignificantly reduced susceptibility of mice overexpressing TGF-α toDSS further substantiates that endogenous TGF-α is a pivotal mediatorof protection and/or healing mechanisms in the colon.
Keywords:transforming growth factor α; epidermal growthfactor; dextran sodium sulphate; colitis; inflammatory bowel disease; transgenic mice |