Specific deletion of Axin1 leads to activation of β-catenin/BMP signaling resulting in fibular hemimelia phenotype in mice

Axin1 的特定缺失导致 β-catenin/BMP 信号激活，从而导致小鼠出现腓骨半肢畸形表型

阅读：6

作者：Rong Xie #, Dan Yi #, Daofu Zeng, Qiang Jie, Qinglin Kang, Zeng Zhang, Zhenlin Zhang, Guozhi Xiao, Lin Chen, Liping Tong, Di Chen

期刊：

Elife

影响因子：

6.400

时间：

2022

起止号：

2022 Dec 21:11:e80013.

doi：

10.7554/eLife.80013

方法学：

研究方向：

信号转导

信号通路：

Wnt/β-Catenin

Abstract

Axin1 is a key regulator of canonical Wnt signaling pathway. Roles of Axin1 in skeletal development and in disease occurrence have not been fully defined. Here, we report that Axin1 is essential for lower limb development. Specific deletion of Axin1 in limb mesenchymal cells leads to fibular hemimelia (FH)-like phenotype, associated with tarsal coalition. Further studies demonstrate that FH disease is associated with additional defects in Axin1 knockout (KO) mice, including decreased osteoclast formation and defects in angiogenesis. We then provide in vivo evidence showing that Axin1 controls limb development through both canonical β-catenin and BMP signaling pathways. We demonstrate that inhibition of β-catenin or BMP signaling could significantly reverse the FH phenotype in mice. Together, our findings reveal that integration of β-catenin and BMP signaling by Axin1 is required for lower limb development. Defect in Axin1 signaling could lead to the development of FH disease.

Specific deletion of Axin1 leads to activation of β-catenin/BMP signaling resulting in fibular hemimelia phenotype in mice

Axin1 的特定缺失导致 β-catenin/BMP 信号激活，从而导致小鼠出现腓骨半肢畸形表型

Abstract

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