Journal
GUT
Volume 52, Issue 7, Pages 981-987Publisher
BMJ PUBLISHING GROUP
DOI: 10.1136/gut.52.7.981
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Introduction: Interleukin 10 knockout (IL-10-/-) mice spontaneously develop a Th1 T cell mediated colitis with many similarities to Crohn's disease. Daily injections of IL-10 are unable to induce remission in mice with established disease. In contrast, we have shown previously that intravenous administration of adenoviral vectors encoding IL-10 ( AdvmuIL-10) induces hepatic IL-10 release and leads to long term disease suppression with profound systemic immunoregulatory changes. Aims: To determine whether rectal delivery of AdvmuIL-10 induces localised colonic IL-10 expression without systemic immune suppression, and assess its therapeutic efficacy in IL-10-/- mice with established colitis. Results: A single rectal infusion of 5 x 10(8) PFU AdvmuIL-10 to 10 week IL-10-/- mice resulted in a median level of 27.3 pg/mg IL-10 in colonic homogenates harvested one week later. IL-10-/- mice with established colitis treated with an enema of 5 x 108 PFU AdvmuIL-10 entered clinical and histological remission whereas empty cassette adenovirus ( Adv0) or phosphate buffered saline ( PBS) treated mice developed progressive disease. After four weeks, the histological score of AdvmuIL-10 treated mice ( 4.4 (1.5)) was significantly lower than that of Adv0 (11.1 (1.1); p< 0.001) and PBS ( 10.9 (1.0); p< 0.01) treated controls. In addition, the stool concentration of IL-1 over the four week experiment was significantly higher in mice treated with saline or Adv0 than in those treated with AdvmuIL-10 ( p< 0.01). Conclusion: Local AdvmuIL-10 therapy reverses colitis in IL-10-/- mice without the systemic effects seen after intravenous administration. Gene therapy strategies using adenoviral vectors encoding immunoregulatory cytokines may prove to be a potent approach to the treatment of chronic inflammatory diseases such as Crohn's disease.
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