软骨内骨化
昼夜节律
生物钟
细胞生物学
内分泌学
内科学
生物
化学
解剖
软骨
医学
作者
Shaoling Yu,Qingming Tang,Guangjin Chen,Xiaofeng Lu,Ying Yin,Mengru Xie,Yanlin Long,Wenhao Zheng,Fengyuan Guo,Longquan Shao,Anbing Shi,Lili Chen
标识
DOI:10.1038/s41418-021-00919-4
摘要
The circadian clock is a master regulator in coordinating daily oscillations of physiology and behaviors. Nevertheless, how the circadian rhythm affects endochondral ossification is poorly understood. Here we showed that endochondral bone formation exhibits circadian rhythms, manifested as fast DNA replication in the daytime, active cell mitosis, and matrix synthesis at night. Circadian rhythm disruption led to endochondral ossification deformities. The mechanistic dissection revealed that melatonin receptor 1 (MTR1) periodically activates the AMPKβ1 phosphorylation, which then orchestrates the rhythms of cell proliferation and matrix synthesis via destabilizing the clock component CRY1 and triggering BMAL1 expression. Accordingly, the AMPKβ1 agonist is capable of alleviating the abnormity of endochondral ossification caused by circadian dysrhythmias. Taken together, these findings indicated that the central circadian clock could control endochondral bone formation via the MTR1/AMPKβ1/BMAL1 signaling axis in chondrocytes. Also, our results suggested that the AMPKβ1 signaling activators are promising medications toward endochondral ossification deformities.
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