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机械敏感蛋白PC1调控破骨细胞及骨吸收的作用机制
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作者 黄梅 周静璇 +20 位作者 李潇骁 刘冉 姜洋子 陈开璇 焦玉睿 尹欣 刘玲 孙宇晨 王维山 肖业 苏甜 郭奇 黄燕 杨觅 魏婕 l.darryl quarles 肖洲生 曾超 罗湘杭 雷光华 李长俊 《Science Bulletin》 SCIE EI CAS CSCD 2024年第12期1964-1979,共16页
Mechanical loading is required for bone homeostasis,but the underlying mechanism is still unclear.Our previous studies revealed that the mechanical protein polycystin-1(PC1,encoded by Pkd1)is critical for bone formati... Mechanical loading is required for bone homeostasis,but the underlying mechanism is still unclear.Our previous studies revealed that the mechanical protein polycystin-1(PC1,encoded by Pkd1)is critical for bone formation.However,the role of PC1 in bone resorption is unknown.Here,we found that PC1directly regulates osteoclastogenesis and bone resorption.The conditional deletion of Pkd1 in the osteoclast lineage resulted in a reduced number of osteoclasts,decreased bone resorption,and increased bone mass.A cohort study of 32,500 patients further revealed that autosomal dominant polycystic kidney disease,which is mainly caused by loss-of-function mutation of the PKD1 gene,is associated with a lower risk of hip fracture than those with other chronic kidney diseases.Moreover,mice with osteoclastspecific knockout of Pkd1 showed complete resistance to unloading-induced bone loss.A mechanistic study revealed that PC1 facilitated TAZ nuclear translocation via the C-terminal tail-TAZ complex and that conditional deletion of Taz in the osteoclast lineage resulted in reduced osteoclastogenesis and increased bone mass.Pharmacological regulation of the PC1-TAZ axis alleviated unloading-and estrogen deficiency-induced bone loss.Thus,the PC1-TAZ axis may be a potential therapeutic target for osteoclast-related osteoporosis. 展开更多
关键词 Polycystin1 OSTEOCLASTOGENESIS Bone resorption Mechanical stress
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