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Intestinal permeability and contractility in murine colitis.

机译:鼠结肠炎的肠道通透性和收缩性。

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摘要

We developed an in vitro organ bath method to measure permeability and contractility simultaneously in murine intestinal segments. To investigate whether permeability and contractility are correlated and influenced by mucosal damage owing to inflammation, BALB/c mice were exposed to a 10% dextran sulphate sodium (DSS) solution for 8 days to induce colitis. The effect of pharmacologically induced smooth muscle relaxation and contraction on permeability was tested in vitro. Regional permeability differences were observed in both control and 10% DSS-treated mice. Distal colon segments were less permeable to 3H-mannitol and 14C-PEG 400 molecules compared with proximal colon and ileum. Intestinal permeability in control vs. 10% DSS mice was not altered, although histologic inflammation score and IFN-gamma pro-inflammatory cytokine levels were significantly increased in proximal and distal colon. IL-1beta levels were enhanced in these proximal and distal segments, but not significantly different from controls. Any effect of pharmacologically induced contractility on intestinal permeability could not be observed. In conclusion, intestinal permeability and contractility are not correlated in this model of experimentally induced colitis in mice. Although simultaneous measurement in a physiological set-up is possible, this method has to be further validated.
机译:我们开发了一种体外器官浸浴方法来同时测量鼠肠段的通透性和收缩性。为了研究通透性和收缩性是否与炎症相关的粘膜损伤相关并受其影响,将BALB / c小鼠暴露于10%的葡聚糖硫酸钠(DSS)溶液中8天,以诱发结肠炎。在体外测试了药理学诱导的平滑肌松弛和收缩对通透性的影响。在对照组和10%DSS处理的小鼠中均观察到区域通透性差异。与近端结肠和回肠相比,远端结肠段对3H-甘露醇和14C-PEG 400分子的渗透性较低。对照组和10%DSS小鼠的肠通透性没有改变,尽管近端和远端结肠的组织学炎症评分和IFN-γ促炎细胞因子水平明显升高。在这些近端和远端节段中,IL-1beta的水平有所提高,但与对照组无明显差异。没有观察到药理学上的收缩力对肠通透性的任何影响。总之,在小鼠实验性结肠炎模型中,肠的通透性和收缩力不相关。尽管可以在生理设置中同时进行测量,但是该方法必须进一步验证。

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