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矿化组织的解剖学与生理学:在骨关节炎发病机制中的作用

Anatomy and physiology of the mineralized tissues: role in the pathogenesis of osteoarthrosis.

作者信息

Burr David B

机构信息

Department of Anatomy and Cell Biology, Biomechanics and Biomaterials Research Center, Indiana University School of Medicine, Indianapolis, Indiana 46202, USA.

出版信息

Osteoarthritis Cartilage. 2004;12 Suppl A:S20-30. doi: 10.1016/j.joca.2003.09.016.

Abstract

Synovial joints are composed of several different kinds of tissue that interact to protect normal joint function. Three subchondral mineralized tissues can be identified-calcified cartilage, subchondral cortical bone, and subchondral trabecular bone-which are distinguished morphologically, physiologically, and mechanically. Each responds to mechanical and pharmaceutical stimuli in different ways through processes of growth, modeling, and remodeling, and changes in each may have a distinct effect on the health of the joint. It is important to distinguish between the structural properties of these tissues and their material properties as these change differently in osteoarthrosis (OA). It is likely that changes in the mineral content and thickness of the calcified cartilage play a greater role in the pathogenesis of OA than has been realized, whereas changes in trabecular bone are probably not causative. Changes in the subchondral cortical bone may accelerate progression of pre-existing disease, but the combined effects of increased subchondral bone turnover and greater subchondral bone volume are not at all clear. Ultimately, the efficacy of bone anti-resorptive therapies for OA will depend upon whether the increased structural stiffness of the subchondral mineralized tissues predisposes the cartilage to deteriorate, whether the increased bone turnover that occurs in OA is itself a causative factor, or whether the lower tissue elastic modulus offsets the increased structural stiffness of the subchondral plate in an attempt to protect the cartilage from damage.

摘要

滑膜关节由几种不同类型的组织组成,这些组织相互作用以保护正常的关节功能。可以识别出三种软骨下矿化组织——钙化软骨、软骨下皮质骨和软骨下小梁骨——它们在形态、生理和力学方面有所不同。每种组织通过生长、塑形和重塑过程以不同方式对机械和药物刺激做出反应,并且每种组织的变化可能对关节健康产生不同的影响。区分这些组织的结构特性和材料特性很重要,因为它们在骨关节炎(OA)中的变化不同。钙化软骨的矿物质含量和厚度变化在OA发病机制中可能比人们意识到的发挥更大作用,而小梁骨的变化可能不是病因。软骨下皮质骨的变化可能会加速已存在疾病的进展,但软骨下骨转换增加和软骨下骨体积增大的综合影响尚不清楚。最终,用于OA的骨抗吸收疗法的疗效将取决于软骨下矿化组织结构刚度的增加是否会使软骨易于退化,OA中发生的骨转换增加本身是否是一个致病因素,或者较低的组织弹性模量是否会抵消软骨下板结构刚度的增加,以试图保护软骨免受损伤。

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