BACKGROUND:We previously demonstrated angiotensin converting enzymes (ACE) over-expression in a dextran-sodium sulfate colitis model; ACE inhibitor (ACE-I) treatment reduced colitis severity in this model. However, ACE-I has not been tested in more immunologically relevant colitis models. AIM:We hypothesized that ACE-I would decrease disease severity in an IL-10 knockout (-/-) colitis model. METHODS:Colitis was induced by giving 10-week old IL-10-/- mice piroxicam (P.O.) for 14 days. The ACE-I enalaprilat was given transanally at a dose of 6.25 mg/kg for 21 days. Prednisolone (PSL) with or without enalaprilat were used as therapeutic, comparative groups. All groups were compared to a placebo treated group. Outcome measures were clinical course, histology, abundance of pro-inflammatory cytokines/chemokines, and epithelial barrier function. RESULTS:Enalaprilat exhibited better survival (91 %) versus other treatment groups (PSL: 85.7 %, PSL + ACE-I: 71.4 %, placebo: 66.6 %). The ACE-I and PSL + ACE-I groups showed significantly better histological scores versus placebo mice. ACE-I and the PSL groups significantly reduced several pro-inflammatory cytokines versus placebo mice. FITC-dextran permeability was reduced in the ACE-I and PSL + ACE-I groups. Blood pressure was not affected in ACE-I treated mice compared to placebo mice. CONCLUSIONS:ACE-I was effective in reducing severity of colitis in an IL-10-/- model. The addition of prednisolone minimally augmented this effect. The findings suggest that appropriately dosed ACE-I with or without steroids may be a new therapeutic agent for colitis.

译文

背景:我们先前证明了在葡聚糖-硫酸钠结肠炎模型中血管紧张素转化酶(ACE)的过度表达。在该模型中,ACEI(ACE-I)抑制剂治疗可降低结肠炎的严重程度。但是,尚未在更具免疫学意义的结肠炎模型中测试ACE-1。
目的:我们假设ACE-1可以降低IL-10基因敲除(-/-)结肠炎模型中的疾病严重程度。
方法:通过给予10周龄的IL-10-/-小鼠吡罗昔康(P.O.)14天来诱发结肠炎。 ACE-1依那普利拉经鼻给药,剂量为6.25 mg / kg,持续21天。泼尼松龙(PSL)有或没有恩那普利拉被用作治疗性比较组。将所有组与安慰剂治疗组进行比较。结果指标包括临床病程,组织学,促炎细胞因子/趋化因子的含量以及上皮屏障功能。
结果:依那普利拉的生存率(91%)优于其他治疗组(PSL:85.7%,PSL ACE-1:71.4%,安慰剂:66.6%)。与安慰剂小鼠相比,ACE-1和PSL ACE-1组的组织学评分明显更高。与安慰剂小鼠相比,ACE-1和PSL组显着减少了几种促炎性细胞因子。在ACE-I和PSL ACE-I组中,FITC-葡聚糖的通透性降低。与安慰剂小鼠相比,ACE-1治疗的小鼠的血压没有受到影响。
结论:ACE-1在降低IL-10-/-模型中结肠炎的严重程度方面有效。泼尼松龙的添加最小程度地增强了这种作用。研究结果表明,适当剂量的ACE-I与或不与类固醇激素可能是结肠炎的一种新的治疗剂。

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