河马信号通路
软骨细胞
雅普1
软骨发生
癌症研究
转录因子
基因敲除
阿格里坎
Wnt信号通路
下调和上调
细胞生长
炎症
MAPK/ERK通路
作者
Yujie Deng,Jinqiu Lu,Wenling Li,Ailing Wu,Xu Zhang,Wenxue Tong,Ki-Wai Kevin Ho,Ling Qin,Hai Song,Kinglun Kingston Mak
标识
DOI:10.1038/s41467-018-07022-2
摘要
Osteoarthritis is one of the leading causes of pain and disability in the aged population due to articular cartilage damage. This warrants investigation of signaling mechanisms that could protect cartilage from degeneration and degradation. Here we show in a murine model of experimental osteoarthritis that YAP activation by transgenic overexpression or by deletion of its upstream inhibitory kinases Mst1/2 preserves articular cartilage integrity, whereas deletion of YAP in chondrocytes promotes cartilage disruption. Our work shows that YAP is both necessary and sufficient for the maintenance of cartilage homeostasis in osteoarthritis. Mechanistically, inflammatory cytokines, such as TNFα or IL-1β, trigger YAP/TAZ degradation through TAK1-mediated phosphorylation. Furthermore, YAP directly interacts with TAK1 and attenuates NF-κB signaling by inhibiting substrate accessibility of TAK1. Our study establishes a reciprocal antagonism between Hippo-YAP/TAZ and NF-κB signaling in regulating the induction of matrix-degrading enzyme expression and cartilage degradation during osteoarthritis pathogenesis.
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