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Signaling pathways effecting crosstalk between cartilage and adjacent tissues: Seminars in cell and developmental biology: The biology and pathology of cartilage

机译:影响软骨与邻近组织之间串扰的信号传导途径:细胞与发育生物学研讨会:软骨的生物学和病理学

摘要

Endochondral ossification, the mechanism responsible for the development of the long bones, is dependent on an extremely stringent coordination between the processes of chondrocyte maturation in the growth plate, vascular expansion in the surrounding tissues, and osteoblast differentiation and osteogenesis in the perichondrium and the developing bone center. The synchronization of these processes occurring in adjacent tissues is regulated through vigorous crosstalk between chondrocytes, endothelial cells and osteoblast lineage cells. Our knowledge about the molecular constituents of these bidirectional communications is undoubtedly incomplete, but certainly some signaling pathways effective in cartilage have been recognized to play key roles in steering vascularization and osteogenesis in the perichondrial tissues. These include hypoxia-driven signaling pathways, governed by the hypoxia-inducible factors (HIFs) and vascular endothelial growth factor (VEGF), which are absolutely essential for the survival and functioning of chondrocytes in the avascular growth plate, at least in part by regulating the oxygenation of developing cartilage through the stimulation of angiogenesis in the surrounding tissues. A second coordinating signal emanating from cartilage and regulating developmental processes in the adjacent perichondrium is Indian Hedgehog (IHH). IHH, produced by pre-hypertrophic and early hypertrophic chondrocytes in the growth plate, induces the differentiation of adjacent perichondrial progenitor cells into osteoblasts, thereby harmonizing the site and time of bone formation with the developmental progression of chondrogenesis. Both signaling pathways represent vital mediators of the tightly organized conversion of avascular cartilage into vascularized and mineralized bone during endochondral ossification.
机译:软骨内骨化是导致长骨发育的机制,它依赖于生长板中软骨细胞成熟过程,周围组织中的血管扩张以及软骨膜和成骨细胞的成骨细胞分化和成骨之间的极为严格的协调骨中心。通过软骨细胞,内皮细胞和成骨细胞谱系细胞之间的强烈串扰来调节在相邻组织中发生的这些过程的同步。我们对这些双向通讯的分子组成的知识无疑是不完整的,但是可以肯定的是,一些有效的软骨信号传导途径在指导软骨膜组织的血管生成和成骨中起着关键作用。这些包括由缺氧诱导因子(HIF)和血管内皮生长因子(VEGF)调控的缺氧驱动信号通路,这些通路对于血管生长板中软骨细胞的存活和功能是绝对必要的,至少部分是通过调节通过刺激周围组织的血管生成来促进软骨的充氧。来自软骨并调节相邻软骨膜中发育过程的第二个协调信号是印度刺猬(IHH)。 IHH由生长前的肥大性和早期肥大性软骨细胞产生,可​​诱导邻近的软骨膜祖细胞分化为成骨细胞,从而使骨形成的部位和时间与软骨形成的发展进程相协调。两种信号通路都代表了软骨内骨化过程中无组织软骨向组织化的矿化血管紧密组织转化的重要介质。

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    Maes Christa;

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  • 年度 2017
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