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体外软骨细胞肥大发育过程中骨相关蛋白、骨钙素和骨桥蛋白的诱导及其基质超微结构定位。

Induction of bone-related proteins, osteocalcin and osteopontin, and their matrix ultrastructural localization with development of chondrocyte hypertrophy in vitro.

作者信息

Lian J B, McKee M D, Todd A M, Gerstenfeld L C

机构信息

Department of Cell Biology, University of Massachusetts Medical Center, Worcester 01655.

出版信息

J Cell Biochem. 1993 Jun;52(2):206-19. doi: 10.1002/jcb.240520212.

Abstract

Endochondral bone formation occurs by a series of developmentally regulated cellular events from initial formation of cartilage tissue to stages of calcified cartilage, resorption, and replacement by bone tissue. Several studies have raised the question of the possibility that the hypertrophic chondrocytes associated with the calcifying cartilage matrix can acquire properties similar to osteoblasts. We have addressed this possibility by measuring synthesis within hypertrophic chondrocytes in vitro of two bone-related proteins, osteopontin and osteocalcin. Chondrocytes derived from chick embryo ventral vertebral tissue were cultured under conditions that promoted extracellular matrix mineralization and differentiation towards the hypertrophic phenotype as indicated by the induction of Type X collagen, alkaline phosphatase, and diminished expression of Type II collagen and the core protein of large proteoglycan. In these cultures, osteopontin synthesis was detected in early cultures in the absence of a calcified matrix; in contrast, an absence of the bone-specific protein osteocalcin was observed. However, with onset of development of the hypertrophic phenotype an induction of protein expression for osteocalcin was observed with a significant (twofold) increase in osteopontin. Maximal levels of osteocalcin synthesis occurred with the peak of alkaline phosphatase activity and Type X collagen mRNA levels. The levels of osteocalcin synthesis were induced fiftyfold from the earliest level of detection but this level was only one one-hundredth of that observed for mature chick osteoblast cultures. Osteocalcin and osteopontin were characterized by several criteria (electrophoresis, immunoblotting, chromatographic characteristics, and response to 1,25(OH)2D3) which confirmed their molecular properties as being identical to osteoblast synthesized proteins. The coordinate change in the cellular phenotype to the hypertrophic chondrocyte was shown to be concurrent with ultrastructural maturation of the cells and the accumulation of osteocalcin and osteopontin in the extracellular matrix associated with hydroxyapatite at sites of mineralization. Since the ultrastructural features of the cells in vitro and the extracellular matrix surrounding the lacunae have features of the hypertrophic chondrocyte and associated matrix in vivo, the induction of the bone-specific protein osteocalcin suggests that at least a population of these cells may develop osteoblastic phenotypic markers in association with mineralizing matrix. The detection of osteocalcin and the high level of synthesis of osteopontin may represent an advanced stage of chondrocyte hypertrophy or the possibility of a trans-differentiation of the chondrocytes to an osteoblastic-like cell.

摘要

软骨内骨形成通过一系列发育调控的细胞事件发生,从软骨组织的初始形成到钙化软骨、吸收以及被骨组织替代的阶段。几项研究提出了这样一个可能性问题,即与钙化软骨基质相关的肥大软骨细胞能否获得类似于成骨细胞的特性。我们通过测量体外肥大软骨细胞中两种骨相关蛋白骨桥蛋白和骨钙素的合成来探讨这种可能性。从鸡胚腹侧椎骨组织分离的软骨细胞在促进细胞外基质矿化并向肥大表型分化的条件下培养,这表现为X型胶原、碱性磷酸酶的诱导以及II型胶原和大蛋白聚糖核心蛋白表达的减少。在这些培养物中,在早期培养且无钙化基质的情况下检测到骨桥蛋白的合成;相反,未观察到骨特异性蛋白骨钙素。然而,随着肥大表型的出现,观察到骨钙素蛋白表达的诱导以及骨桥蛋白显著(两倍)增加。骨钙素合成的最大水平出现在碱性磷酸酶活性和X型胶原mRNA水平的峰值时。骨钙素合成水平从最早检测水平诱导增加了五十倍,但该水平仅为成熟鸡成骨细胞培养物中观察到水平的百分之一。通过几种标准(电泳、免疫印迹、色谱特征以及对1,25(OH)2D3的反应)对骨钙素和骨桥蛋白进行了表征,这些标准证实它们的分子特性与成骨细胞合成的蛋白质相同。细胞表型向肥大软骨细胞的协同变化显示与细胞的超微结构成熟以及骨钙素和骨桥蛋白在矿化部位与羟基磷灰石相关的细胞外基质中的积累同时发生。由于体外细胞和围绕腔隙的细胞外基质的超微结构特征具有体内肥大软骨细胞和相关基质的特征,骨特异性蛋白骨钙素的诱导表明这些细胞中至少有一部分可能在与矿化基质相关的情况下发展出成骨细胞表型标记。骨钙素的检测以及骨桥蛋白的高水平合成可能代表软骨细胞肥大的晚期阶段或软骨细胞向成骨样细胞转分化的可能性。

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