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Effect of ectopic expression of rat trefoil factor family 3 (intestinal trefoil factor) in the jejunum of transgenic mice

机译:大鼠三叶因子家族3(肠三叶因子)在转基因小鼠空肠中异位表达的影响

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摘要

To further examine the function of the trefoil factor family (TFF), the expression of which is up-regulated at sites of injury, we have produced transgenic mice that chronically express rat TFF3 within the jejunum (using a rat fatty acid-binding protein promoter). The expression of rat TFF3 was limited to the villi of the jejunum and had no effect on base-line morphology. Rat TFF3 expression did result, however, in a reduced sensitivity to indomethacin (85 mg/kg sulbcutaneously), which only caused a 29% reduction in villus height in transgenics versus 51% reduction in controls (p <0.01). Indomethacin increased initial intestinal epithelial cell proliferation and migration, but the presence of rat TFF3 caused no additional change in proliferation (bromodeoxyuridine), cell migration ([H-3]thymidine and bromodeoxyuridine), apoptosis (terminal deoxyuridine nucleotidyl nick end labeling), or E-cadherin immunostaining, In vitro studies following changes in resistance of intestinal strips in Ussing chambers (voltage-clamp technique) showed increased base-line resistance in the rat TFF3-expressing region (326 +/- 60 versus 195 +/- 48 ohm.cm(2) in controls, p <0.05) and reduced the fall in resistance following Hel exposure by about 40% (p <0.01). Overexpression of TFF3 stabilizes the mucosa against noxious agents, supporting its role in mucosal protection/repair. It may therefore provide a novel approach to the prevention and/or treatment of intestinal ulceration.
机译:为了进一步检查三叶因子家族(TFF)的功能,该表达在损伤部位上调,我们生产了在空肠内长期表达大鼠TFF3的转基因小鼠(使用大鼠脂肪酸结合蛋白启动子)。大鼠TFF3的表达仅限于空肠绒毛,对基线形态无影响。但是,大鼠TFF3表达确实导致了对消炎痛的敏感性降低(皮肤经皮85 mg / kg),这仅使转基因动物的绒毛高度降低了29%,而对照组则降低了51%(p <0.01)。消炎痛增加了初始肠上皮细胞的增殖和迁移,但是大鼠TFF3的存在没有引起增殖(溴脱氧尿苷),细胞迁移([H-3]胸苷和溴脱氧尿苷),细胞凋亡(末端脱氧尿苷核苷酸末端标记)的其他变化,或E-cadherin免疫染色,在Ussing小室中肠条电阻变化后的体外研究(电压钳技术)显示,大鼠TFF3表达区的基线电阻增加(326 +/- 60对195 +/- 48 ohm)对照组中的.cm(2),p <0.05),并且在Hel暴露后的电阻下降降低了约40%(p <0.01)。 TFF3的过表达稳定了粘膜抵抗有害物质,支持其在粘膜保护/修复中的作用。因此,它可以提供预防和/或治疗肠道溃疡的新颖方法。

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