多细胞生物
群众
联轴节(管道)
吸收
单位(环理论)
骨形成
生物
医学
病理
工程类
心理学
内分泌学
遗传学
细胞
机械工程
认识论
哲学
数学教育
作者
Natalie A. Sims,T. John Martin
出处
期刊:BoneKEy reports
[Portico]
日期:2014-01-08
卷期号:3: 481-481
被引量:689
标识
DOI:10.1038/bonekey.2013.215
摘要
Coupling between bone formation and bone resorption refers to the process within basic multicellular units in which resorption by osteoclasts is met by the generation of osteoblasts from precursors, and their bone-forming activity, which needs to be sufficient to replace the bone lost. There are many sources of activities that contribute to coupling at remodeling sites, including growth factors released from the matrix, soluble and membrane products of osteoclasts and their precursors, signals from osteocytes and from immune cells and signaling taking place within the osteoblast lineage. Coupling is therefore a process that involves the interaction of a wide range of cell types and control mechanisms. As bone remodeling occurs at many sites asynchronously throughout the skeleton, locally generated activities comprise very important control mechanisms. In this review, we explore the potential roles of a number of these factors, including sphingosine-1-phosphate, semaphorins, ephrins, interleukin-6 (IL-6) family cytokines and marrow-derived factors. Their interactions achieve the essential tight control of coupling within individual remodeling units that is required for control of skeletal mass.
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