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首页> 外文期刊>Journal of Gastrointestinal Surgery >Development of a Simple Model of Extrinsic Denervation of the Small Bowel in Mouse
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Development of a Simple Model of Extrinsic Denervation of the Small Bowel in Mouse

机译:小鼠小肠外源性去神经支配简单模型的建立

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Small bowel transplantation (SBT) is associated with poorly understood enteric dysfunction. The study of SBT in mice is hindered by the technical difficulty of orthotopic SBT in the mouse. Our aim was to develop an easy preparation of extrinsic denervation of the entire jejunoileum in mice as a model of orthotopic SBT. All neurolymphatic tissues accompanying the superior mesenteric artery (SMA) and vein (SMV) were ligated just distal to the middle colic vessels. The SMA and SMV were then stripped of investing adventitia, and the mesentery to jejunum and colon were transected radially. Jejunum and colon were not transected and reanastomosed. To confirm extrinsic denervation 1, 3, and 6 months later, segments of small bowel were stained for protein gene product 9.5 (PGP9.5) and tyrosine hydroxylase (TH). Tyrosine hydroxylase immunoreactive intensity was then quantified using a semiquantitative analysis. Immunohistochemical fluorescence showed persistence of PGP9.5 immunoreactivity confirming enteric nerves in jejunoileum; however, there was no TH immunoreactivity in jejunoileum in denervated mice despite the expected preservation of TH immunoreactivity in the still-innervated duodenum at 1 month. At 3 months, sparse immunoreactivity for TH was present, and by 6 months, reinnervation of TH-containing nerves appeared similar to controls. Quantification of intensity at each time-point further confirmed this trend. This technique in the mouse accomplishes a complete extrinsic denervation of jejunoileum early postoperatively (1 and 3 months); reinnervation occurs by 6 months. This is an easily learned murine model of orthotopic SBT.
机译:小肠移植(SBT)与人们对肠功能障碍的了解程度不高有关。小鼠原位SBT的技术难度阻碍了小鼠SBT的研究。我们的目的是作为原位SBT的模型开发一种易于制备的小鼠整个空肠外源性去神经的方法。结扎肠系膜上动脉(SMA)和静脉(SMV)的所有神经淋巴组织正好位于结肠中部血管的远端。然后去除SMA和SMV的外膜,并径向切开空肠和结肠的肠系膜。空肠和结肠未切除并重新吻合。为了确认外在神经支配的1、3和6个月后,对小肠段进行了蛋白基因产物9.5(PGP9.5)和酪氨酸羟化酶(TH)染色。然后使用半定量分析定量酪氨酸羟化酶的免疫反应强度。免疫组织化学荧光显示PGP9.5免疫反应持续存在,确认空肠肠神经。然而,尽管预期在1个月仍在神经支配的十二指肠中保留TH免疫反应性,但在失神经小鼠中空肠回肠中没有TH免疫反应性。在3个月时,TH的免疫反应稀疏,到6个月时,含TH的神经的神经支配似乎与对照组相似。在每个时间点强度的量化进一步证实了这种趋势。小鼠中的这项技术可在术后早期(1和3个月)完成空肠完全外在神经支配。再神经发生在6个月之前。这是原位SBT的易于学习的小鼠模型。

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