Department of Pediatrics, National Jewish Health, Denver, CO80206, USA.
Am J Pathol. 2011 Jul;179(1):367-79. doi: 10.1016/j.ajpath.2011.03.016. Epub 2011 May 5.
The purpose of this study was to determine whether β-catenin regulates basal cell fate determination in the mouse trachea. Analysis of TOPGal transgene reporter activity and Wnt/β-catenin pathway gene expression suggested a role for β-catenin in basal cell proliferation and differentiation after naphthalene-mediated Clara-like and ciliated cell depletion. However, these basal cell activities occurred simultaneously, limiting precise determination of the role(s) played by β-catenin. This issue was overcome by analysis of β-catenin signaling in tracheal air-liquid interface cultures. The cultures could be divided into two phases: basal cell proliferation and basal cell differentiation. A role for β-catenin in basal cell proliferation was indicated by activation of the TOPGal transgene on proliferation days 3 to 5 and by transient expression of Myc (alias c-myc). Another peak of TOPGal transgene activity was detected on differentiation days 2 to 10 and was associated with the expression of Axin 2. These results suggest a role for β-catenin in basal to ciliated and basal to Clara-like cell differentiation. Genetic stabilization of β-catenin in basal cells shortened the period of basal cell proliferation but had a minor effect on this process. Persistent β-catenin signaling regulated basal cell fate by driving the generation of ciliated cells and preventing the production of Clara-like cells.
本研究旨在确定β-连环蛋白是否调节小鼠气管中的基底细胞命运决定。TOPGal 转基因报告基因活性和 Wnt/β-连环蛋白信号通路基因表达分析表明,β-连环蛋白在萘介导的 Clara 样细胞和纤毛细胞耗竭后参与基底细胞增殖和分化。然而,这些基底细胞活性同时发生,限制了β-连环蛋白所起作用的确切确定。通过气管气液界面培养物中β-连环蛋白信号的分析克服了这个问题。该培养物可分为两个阶段:基底细胞增殖和基底细胞分化。TOPGal 转基因在增殖第 3 至 5 天的激活以及 Myc(别名 c-myc)的瞬时表达表明β-连环蛋白在基底细胞增殖中的作用。在分化第 2 至 10 天还检测到另一个 TOPGal 转基因活性峰,与 Axin 2 的表达相关。这些结果表明β-连环蛋白在基底细胞向纤毛细胞和基底细胞向 Clara 样细胞分化中起作用。在基底细胞中稳定遗传β-连环蛋白缩短了基底细胞增殖的时间,但对该过程的影响较小。持续的β-连环蛋白信号通过驱动纤毛细胞的产生并防止 Clara 样细胞的产生来调节基底细胞命运。
