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成年大鼠骨髓细胞体外形成矿化组织相关骨基质蛋白的表达:地塞米松对成骨细胞表型的诱导作用

Expression of bone matrix proteins associated with mineralized tissue formation by adult rat bone marrow cells in vitro: inductive effects of dexamethasone on the osteoblastic phenotype.

作者信息

Kasugai S, Todescan R, Nagata T, Yao K L, Butler W T, Sodek J

机构信息

Medical Research Council Group in Periodontal Physiology, Faculty of Dentistry, University of Toronto, Ontario, Canada.

出版信息

J Cell Physiol. 1991 Apr;147(1):111-20. doi: 10.1002/jcp.1041470115.

Abstract

The nature and tissue distribution of non-collagenous bone proteins synthesized by adult rat bone marrow cells, induced to differentiate in the presence of dexamethasone (DEX) and beta-glycerophosphate (beta-GP), was studied in vitro to determine the potential role of these proteins in bone formation. Northern hybridization analysis revealed a strong induction of bone sialoprotein (BSP) and osteocalcin in DEX-treated cultures, whereas the constitutive expression of secreted phosphoprotein I (SPP-1), type I collagen, SPARC, and alkaline phosphatase was stimulated 6-, 5-, 3-, and 2.5-told, respectively. Metabolic labeling of proteins showed that the sialoproteins (SPP-1 and BSP) were mostly secreted into the culture medium in the non-mineralizing (-beta-GP) cultures, but were the predominant non-collagenous proteins associated with the hydroxyapatite of the bone nodules in mineralizing cultures (+ beta-GP). Extraction of the tissue matrix with 4 M GuHCl and digestion of the demineralized tissue matrix with bacterial collagenase revealed that some BSP was also associated non-covalently and covalently with the collagenous matrix. SPP-1 was present in two distinct, 44 kDa and 55 kDa, forms in the conditioned medium of all cultures and was preferentially associated with the hydroxyapatite in the mineralizing cultures. In comparison, SPARC was abundant in culture media but could not be detected in de-mineralizing extracts of the mineralized tissue. Radiolabeling with [35SO4] demonstrated that both SPP-1 and BSP synthesized by bone cells are sulfated, and that a 35 kDa protein and some proteoglycan were covalently associated with the collagenous matrix in +DEX cultures. Labeling with [32PO4] was essentially confined to the sialoproteins; the 44 kDa SPP-1 incorporating significantly more [32PO4] than the 55 kDa SPP-1 and the BSP. These studies demonstrate that BSP and osteocalcin are only expressed in differentiated osteoblasts and that most of the major non-collagenous bone proteins associate with the bone mineral. However, some novel proteins together with some of the BSP are associated with the collagenous matrix where they can influence hydroxyapatite formation.

摘要

研究了成年大鼠骨髓细胞在地塞米松(DEX)和β-甘油磷酸酯(β-GP)存在下诱导分化合成的非胶原蛋白的性质和组织分布,以确定这些蛋白质在骨形成中的潜在作用。Northern杂交分析显示,在DEX处理的培养物中骨唾液蛋白(BSP)和骨钙素强烈诱导,而分泌性磷蛋白I(SPP-1)、I型胶原、SPARC和碱性磷酸酶的组成型表达分别被刺激6倍、5倍、3倍和2.5倍。蛋白质的代谢标记显示,在非矿化(-β-GP)培养物中,唾液蛋白(SPP-1和BSP)大多分泌到培养基中,但在矿化培养物(+β-GP)中是与骨结节羟基磷灰石相关的主要非胶原蛋白。用4M盐酸胍提取组织基质并用细菌胶原酶消化脱矿化组织基质表明,一些BSP也以非共价和共价方式与胶原基质相关。SPP-1在所有培养物的条件培养基中以两种不同的形式存在,即44kDa和55kDa,并且在矿化培养物中优先与羟基磷灰石相关。相比之下,SPARC在培养基中含量丰富,但在矿化组织的脱矿化提取物中未检测到。用[35SO4]进行放射性标记表明,骨细胞合成的SPP-1和BSP都被硫酸化,并且在+DEX培养物中,一种35kDa的蛋白质和一些蛋白聚糖与胶原基质共价相关。用[32PO4]标记基本上仅限于唾液蛋白;44kDa的SPP-1比55kDa的SPP-1和BSP掺入的[32PO4]明显更多。这些研究表明,BSP和骨钙素仅在分化的成骨细胞中表达,并且大多数主要的非胶原蛋白与骨矿物质相关。然而,一些新的蛋白质以及一些BSP与胶原基质相关,在那里它们可以影响羟基磷灰石的形成。

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