- 作者:Jasreen Kular ; Jennifer Tickner ; Shek Man Chim ; Jiake Xu
- 关键词:Osteoclast ; Osteoblast ; Osteocyte ; Osteomac ; Bone lining cell ; Bone remodelling ; Coupling factors ; Endothelial cell ; RANKL ; Osteoporosis
- 刊名:Clinical Biochemistry
- 出版年:2012
- 出版时间:August, 2012
- 年:2012
- 卷:45
- 期:12
- 页码:863-873
- 全文大小:737 K
Objectives
To review the current literature on the regulation of bone remodelling at the cellular level.Design and methods
The cellular activities of the cells in the basic multicellular unit (BMU) were evaluated.
Results
Bone remodelling requires an intimate cross-talk between osteoclasts and osteoblasts and is tightly coordinated by regulatory proteins that interact through complex autocrine/paracrine mechanisms. Osteocytes, bone lining cells, osteomacs, and vascular endothelial cells also regulate bone remodelling in the BMU via cell signalling networks of ligand-receptor complexes. In addition, through secreted and membrane-bound factors in the bone microenvironment, T and B lymphocytes mediate bone homeostasis in osteoimmunology.
Conclusions
Osteoporosis and other bone diseases occur because multicellular communication within the BMU is disrupted. Understanding the cellular and molecular basis of bone remodelling and the discovery of novel paracrine or coupling factors, such as RANKL, sclerostin, EGFL6 and semaphorin 4D, will lay the foundation for drug development against bone diseases.