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Establishment and evaluation of an experimental rat model for high-altitude intestinal barrier injury

机译:大鼠高原肠屏障损伤模型的建立与评价

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摘要

In the present study an experimental high-altitude intestinal barrier injury rat model was established by simulating an acute hypoxia environment, to provide an experimental basis to assess the pathogenesis, prevention and treatment of altitude sickness. A total of 70 healthy male Sprague-Dawley rats were divided into two groups: Control group (group C) and a high-altitude hypoxia group (group H). Following 2 days adaptation, the rats in group H were exposed to a simulated 4,000-m, high-altitude hypoxia environment for 3 days to establish the experimental model. To evaluate the model, bacterial translocation, serum lipopolysaccharide level, pathomorphology, ultrastructure and protein expression in rats were assessed. The results indicate that, compared with group C, the rate of bacterial translocation and the apoptotic index of intestinal epithelial cells were significantly higher in group H (P<0.01). Using a light microscope it was determined that the intestinal mucosa was thinner in group H, there were fewer epithelial cells present and the morphology was irregular. Observations with an electron microscope indicated that the intestinal epithelial cells in group H were injured, the spaces among intestinal villi were wider, the tight junctions among cells were open and lanthanum nitrate granules (from the fixing solution) had diffused into the intestinal mesenchyme. The expression of the tight junction protein occludin was also decreased in group H. Therefore, the methods applied in the present study enabled the establishment of a stable, high-altitude intestinal barrier injury model in rats.
机译:本研究通过模拟急性缺氧环境建立了实验性高空肠屏障损伤大鼠模型,为评估高原反应的发病机理,预防和治疗提供了实验依据。将总共​​70只健康的雄性Sprague-Dawley大鼠分为两组:对照组(C组)和高海拔缺氧组(H组)。适应2天后,将H组的大鼠暴露于模拟的4,000 m的高海拔缺氧环境中3天,以建立实验模型。为了评估模型,评估了大鼠的细菌移位,血清脂多糖水平,病理形态,超微结构和蛋白质表达。结果表明,与C组相比,H组的细菌移位率和肠上皮细胞凋亡指数均显着升高(P <0.01)。使用光学显微镜确定,H组的肠粘膜较薄,上皮细胞较少,形态不规则。电镜观察表明,H组肠上皮细胞受到损伤,肠绒毛之间的间隙变宽,细胞间的紧密连接开放,硝酸镧颗粒(来自固定液)扩散到肠间质中。 H组紧密连接蛋白occludin的表达也降低。因此,本研究中使用的方法能够建立大鼠稳定,高空肠屏障损伤模型。

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