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矿化组织中细胞与其基质的界面:综述

The interface of cells and their matrices in mineralized tissues: a review.

作者信息

Jones S J, Boyde A, Ali N N

出版信息

Scan Electron Microsc. 1986(Pt 4):1555-69.

PMID:3810026
Abstract

The interface between cells and matrices in mineralized tissues formed in vivo has been studied mainly by looking at the matrix surface, which is easily prepared, and not at the cell surface, which presents problems. Vertebrate calcified tissues range from being acellular to highly cellular, but for all the tissues the formative cells lay down and organise a cell-specific matrix, although this may be deposited initially on a different tissue-type. The formation of hard tissues is a group activity of many cells; resorption is the province of one cell, though it may be controlled by others in the vicinity. Cell-matrix interfaces that develop in vitro have also mainly been studied at the matrix side. The main difficulty with in vitro studies of hard tissue interfaces is that the cells do not have the same activity or even cellular functions as they had in vivo under the complex control of physiological regulation. The question of osteoblastic osteoclasis falls into this category. It is possible to provide new substrata for both formative and resorptive hard tissue cells to test for the interaction between the cells and the 'matrix' on to which they are seeded. The changing cell-matrix interface may also be modelled using computer simulation of osteoclastic movement across a substrate based on known patterns exhibited by other cell types in vitro. Comparison with the shapes of complex resorption pits shows a surprising match. This suggests that the track of the osteoclast due to cell motility and the bone resorptive mechanism resulting in pits along that track are likely to be separately controlled phenomena.

摘要

体内形成的矿化组织中细胞与基质之间的界面,主要是通过观察易于制备的基质表面来进行研究的,而非存在问题的细胞表面。脊椎动物的钙化组织从无细胞到高度细胞化不等,但对于所有这些组织而言,形成细胞都会分泌并组织一种细胞特异性基质,尽管这种基质最初可能沉积在不同的组织类型上。硬组织的形成是许多细胞的集体活动;吸收则是单个细胞的职责范围,尽管它可能受到附近其他细胞的控制。体外形成的细胞 - 基质界面也主要是在基质一侧进行研究的。硬组织界面体外研究的主要困难在于,在生理调节的复杂控制下,细胞在体外并不具有与体内相同的活性甚至细胞功能。成骨破骨作用问题就属于这一范畴。有可能为形成性和吸收性硬组织细胞提供新的基质,以测试细胞与它们所接种的“基质”之间的相互作用。基于体外其他细胞类型所呈现的已知模式,通过计算机模拟破骨细胞在基质上的移动,也可以对不断变化的细胞 - 基质界面进行建模。与复杂吸收凹坑形状的比较显示出惊人的匹配。这表明,由于细胞运动性导致的破骨细胞轨迹以及沿该轨迹形成凹坑的骨吸收机制,可能是分别受控的现象。

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