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骨、牙齿和骨整合植入物矿化组织界面处的骨桥蛋白:超微结构分布及其对矿化组织形成、更新和修复的影响

Osteopontin at mineralized tissue interfaces in bone, teeth, and osseointegrated implants: ultrastructural distribution and implications for mineralized tissue formation, turnover, and repair.

作者信息

McKee M D, Nanci A

机构信息

Department of Stomatology, Université de Montréal, Quebec, Canada.

出版信息

Microsc Res Tech. 1996 Feb 1;33(2):141-64. doi: 10.1002/(SICI)1097-0029(19960201)33:2<141::AID-JEMT5>3.0.CO;2-W.

Abstract

Currently available data describing the gene expression and regulation, secretion, distribution, and protein chemistry of osteopontin (OPN) all are consistent with the notions of this protein functioning as an inhibitor of mineralization and/or as a mediator of cell-matrix and matrix-matrix/mineral adhesion (cohesion) during the formation, turnover, and repair of normal and pathological mineralized tissues. The properties and overall integrity of mineralized tissues are in part dictated by the nature of their interfaces--sites where organic and inorganic components of the extracellular matrix interact to provide biomechanical strength, regulate mineral ion homeostasis, and influence cellular events involved in mineralized tissue modeling, remodeling, and repair. High-resolution, colloidal-gold immunocytochemistry has been used to characterize the proteinaceous composition of these interfaces and to establish that the phosphorylated sialoprotein, OPN, is a major component found at these sites where it accumulates as a dense, planar "coating" of organic material termed either a cement line or a lamina limitans. Structural/functional features of OPN predict an ability of this protein to regulate calcification in the matrix proper of mineralized tissues and to participate, more specifically, in cell-matrix and matrix-matrix/mineral adhesion in laminae limitantes and cement lines, respectively. From the ultrastructural immunocytochemical data presented herein for OPN illustrating the cellular expression and extracellular matrix distribution of this protein, it is demonstrated that the production of OPN is one of the earliest, and latest, secretory activities of the osteoblast lineage and that this activity manifests itself morphologically as a cement line or a lamina limitans, respectively, at bone matrix interfaces. In laminae limitantes at bone surfaces, OPN appears to be involved in osteoclast adhesion and possibly haptotaxis. An OPN-containing cement line is also present at hard tissue interfaces in rat tooth, against osseointegrated titanium and hydroxyapatite implants and at the margins of surgically created bone defects--and there may influence biological adhesion in a manner similar to that proposed for normal bone. It is suggested, therefore, that in addition to its potential for influencing cell adhesion/dynamics in bones and teeth, OPN in cement lines may act as an interfacial adhesion promoter between apposing substrates, therein maintaining the overall integrity of bone during the bone remodeling sequence and "bonding" dissimilar tissues (or biocompatible materials) together in biological composites such as teeth and osseointegrated implants.

摘要

目前可得的关于骨桥蛋白(OPN)的基因表达与调控、分泌、分布及蛋白质化学的资料均与以下观点一致:在正常和病理性矿化组织的形成、更新及修复过程中,该蛋白质作为矿化抑制剂和/或作为细胞-基质以及基质-基质/矿物质黏附(凝聚)的介质发挥作用。矿化组织的特性及整体完整性部分取决于其界面的性质,即细胞外基质的有机和无机成分相互作用以提供生物力学强度、调节矿质离子稳态并影响参与矿化组织建模、重塑及修复的细胞活动的位点。高分辨率胶体金免疫细胞化学已用于表征这些界面的蛋白质组成,并证实磷酸化唾液酸蛋白OPN是在这些位点发现的主要成分,它以致密的平面“涂层”形式积累,这种有机材料层被称为黏合线或限制板。OPN的结构/功能特征预示该蛋白质有能力调节矿化组织基质中的钙化,并更具体地分别参与限制板和黏合线中的细胞-基质以及基质-基质/矿物质黏附。从本文给出的OPN超微结构免疫细胞化学数据显示该蛋白质的细胞表达和细胞外基质分布来看,已证明OPN的产生是成骨细胞谱系最早和最晚的分泌活动之一,且这种活动在形态学上分别表现为骨基质界面处的黏合线或限制板。在骨表面的限制板中,OPN似乎参与破骨细胞黏附并可能参与趋触性。含OPN的黏合线也存在于大鼠牙齿的硬组织界面、与骨结合的钛和羟基磷灰石植入物处以及手术造成的骨缺损边缘,并且可能以类似于正常骨的方式影响生物黏附。因此有人提出,除了其影响骨骼和牙齿中细胞黏附/动态的潜力外,黏合线中的OPN可能作为相邻底物之间的界面黏附促进剂,从而在骨重塑过程中维持骨的整体完整性,并在生物复合材料如牙齿和骨结合植入物中将不同组织(或生物相容性材料)“结合”在一起。

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