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Differential effects of transforming growth factor-beta on the synthesis of extracellular matrix proteins by normal fetal rat calvarial bone cell populations

机译:转化生长因子-β对正常胎鼠颅骨骨细胞群细胞外基质蛋白合成的差异作用

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摘要

To determine the effects of transforming growth factor-beta (TGF-beta) on the different cell types that exist in bone, cell populations (I- IV), progressively enriched in osteoblastic cells relative to fibroblastic cells, were prepared from fetal rat calvaria using timed collagenase digestions. TGF-beta did not induce anchorage-independent growth of these cells, nor was anchorage-dependent growth stimulated in most populations studied, despite a two- to threefold increase in the synthesis of cellular proteins. In all populations the synthesis of secreted proteins increased 2-3.5-fold. In particular, collagen, fibronectin, and plasminogen activator inhibitor synthesis was stimulated. However, different degrees of stimulation of individual proteins were observed both within and between cell populations. A marked preferential stimulation of plasminogen activator inhibitor was observed in each population, together with a slight preferential stimulation of collagen; the effect on collagen expression being directed primarily at type I collagen. In contrast, the synthesis of SPARC (secreted protein acidic rich in cysteine/osteonectin was stimulated approximately two-fold by TGF-beta, but only in fibroblastic populations. Collectively, these results demonstrate that TGF-beta stimulates matrix production by bone cells and, through differential effects on individual matrix components, may also influence the nature of the matrix formed by different bone cell populations. In the presence of TGF-beta, osteoblastic cells lost their polygonal morphology and alkaline phosphatase activity was decreased, reflecting a suppression of osteoblastic features. The differential effects of TGF- beta on bone cell populations are likely to be important in bone remodeling and fracture repair.
机译:为了确定转化生长因子-β(TGF-β)对骨骼中不同细胞类型的影响,使用胎鼠颅盖法制备了相对于成纤维细胞逐渐富集成骨细胞的细胞群(I-IV),定时胶原酶消化。尽管大多数细胞蛋白的合成增加了2到3倍,但TGF-β并未诱导这些细胞的依赖于贴壁的生长,也没有刺激依赖于贴壁的生长。在所有种群中,分泌蛋白的合成增加了2-3.5倍。特别地,刺激了胶原蛋白,纤连蛋白和纤溶酶原激活剂抑制剂的合成。但是,在细胞群内和细胞群之间都观察到了不同程度的单个蛋白质刺激。在每个人群中均观察到纤溶酶原激活剂抑制剂的明显优先刺激,以及胶原蛋白的轻微优先刺激。对胶原蛋白表达的影响主要针对I型胶原蛋白。相比之下,TARC-β刺激SPARC(酸性富含半胱氨酸/骨连接蛋白的分泌蛋白的合成)受到大约两倍的刺激,但仅在成纤维细胞群体中受到刺激。总的来说,这些结果表明TGF-β刺激骨细胞产生基质,并且通过对各个基质成分的不同影响,也可能影响由不同骨细胞群体形成的基质的性质。在存在TGF-β的情况下,成骨细胞失去了多边形形态,碱性磷酸酶活性降低,反映了成骨细胞功能的抑制TGF-β对骨细胞群的不同作用可能在骨重塑和骨折修复中很重要。

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