Section of Pediatric Surgery, Department of Surgery, University of Michigan Health System , Ann Arbor, Michigan.
Tissue Eng Part A. 2014 Feb;20(3-4):830-41. doi: 10.1089/ten.TEA.2013.0383. Epub 2013 Nov 6.
Novel strategies are needed to address the problem of patients with short bowel syndrome. We previously demonstrated a three-fold lengthening of pig bowel after 2 weeks of applied distractive forces, but we have not elucidated the mechanisms facilitating this growth. We used a mouse model of distraction-induced enterogenesis. High molecular weight polyethylene glycol (PEG) osmotically stretched an isolated small bowel segment (PEG-stretch). Significant increases in villus height and crypt depth and in intestinal epithelial cell length and numbers suggested epithelial remodeling in addition to proliferation during enterogenesis. LC-MS/MS analysis showed a two-fold upregulation of α-actinin-1 and -4. We also demonstrated that p-focal adhesion kinase (FAK), FAK, α-actinin, and Rac1 were significantly upregulated and that F-actin was relocalized in PEG-stretch versus controls. Blockade of the phosphotidyl inositol 3' kinase pathway failed to influence the increase in proliferation or decline in apoptosis after stretch, suggesting alternative signaling pathways are used, including MEK and P38MAPK, which were both upregulated during enterogenesis. Our data suggests that several known mechanotransduction pathways drive distraction-induced enterogenesis.
需要新的策略来解决短肠综合征患者的问题。我们之前证明了施加牵拉力量 2 周后,猪肠的长度可以延长三倍,但我们尚未阐明促进这种生长的机制。我们使用了一种牵拉诱导肠发生的小鼠模型。高分子量聚乙二醇(PEG)通过渗透压拉伸一个分离的小肠段(PEG 拉伸)。绒毛高度、隐窝深度以及肠上皮细胞长度和数量的显著增加表明,除了增殖之外,上皮细胞还发生了重塑。LC-MS/MS 分析显示 α-辅肌动蛋白-1 和 -4 的表达上调了两倍。我们还证明,p-黏着斑激酶(FAK)、FAK、α-辅肌动蛋白和 Rac1 的表达显著上调,并且 F-肌动蛋白在 PEG 拉伸与对照组中的重定位。PI3K 通路的磷酸化阻断未能影响拉伸后增殖的增加或凋亡的减少,这表明使用了替代的信号通路,包括 MEK 和 P38MAPK,它们在肠发生过程中均上调。我们的数据表明,几种已知的机械转导途径驱动牵拉诱导肠发生。
