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Bmp4 is required for tracheal formation: a novel mouse model for tracheal agenesis.

机译:Bmp4是气管形成所必需的:一种用于气管再生的新型小鼠模型。

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Tracheal agenesis/atresia (TA) is a rare but fatal congenital disease in which the breathing tube fails to grow. The etiology of this serious condition remains largely unknown. We found that Bmp signaling is prominently present in the anterior foregut where the tracheal primordium originates and targeted ablation of Bmp4 (Bmp4(cko)) resulted in a loss-of-trachea phenotype that closely resembles the Floyd type II pathology, the most common form of TA in humans. In Bmp4(cko) embryos, tracheal specification was not affected; however, its outgrowth was severely impaired due to reduced epithelial and mesenchymal proliferation. In agreement, we also observed significant reduction in the expression of Cyclin D1, a key cell cycle regulator associated with cellular proliferation. However, the proliferative effect of Bmp signaling appears to be independent of Wnt signaling. Interestingly, we found significantly reduced expression of activated extracellular signal-regulated kinase (Erk) in the Bmp4(cko) ventral foregut, suggesting that Bmp signaling promotes Erk phosphorylation which has been associated with cellular proliferation. This study provides the first evidence linking Bmp signaling to tracheal formation by regulating the proliferative response of the anterior ventral foregut. Our finding sheds light on human tracheal malformations by providing a novel mouse model implicating Bmp signaling, non-canonical Erk activation and cellular proliferation.
机译:气管发育不全/闭锁(TA)是一种罕见但致命的先天性疾病,其中呼吸管无法生长。这种严重疾病的病因学仍然未知。我们发现Bmp信号显着存在于气管原基起源的前前肠中,Bmp4的靶向消融(Bmp4(cko))导致气管丢失表型,非常类似于弗洛伊德II型病理,这是最常见的形式在人类中的TA。在Bmp4(cko)胚胎中,气管规格没有受到影响。然而,由于上皮和间充质增殖减少,其生长严重受损。一致地,我们还观察到细胞周期蛋白D1(与细胞增殖相关的关键细胞周期调节因子)的表达显着降低。但是,Bmp信号的增殖效应似乎与Wnt信号无关。有趣的是,我们发现Bmp4(cko)腹侧前肠中活化的细胞外信号调节激酶(Erk)的表达显着降低,这表明Bmp信号传导促进了与细胞增殖相关的Erk磷酸化。这项研究提供了第一个证据,通过调节前腹前肠的增殖反应,将Bmp信号传导与气管形成联系起来。我们的发现通过提供涉及Bmp信号传导,非经典Erk激活和细胞增殖的新型小鼠模型,揭示了人类气管畸形。

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