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在小鼠胚胎成骨过程中,骨钙素1(STC1)蛋白和信使核糖核酸(mRNA)受发育调控:stc1作为成骨细胞发育和骨形成的自分泌/旁分泌因子的潜力。

Stanniocalcin 1 (STC1) protein and mRNA are developmentally regulated during embryonic mouse osteogenesis: the potential of stc1 as an autocrine/paracrine factor for osteoblast development and bone formation.

作者信息

Yoshiko Yuji, Aubin Jane E, Maeda Norihiko

机构信息

Department of Anatomy, Hiroshima University Faculty of Dentistry, Minami-ku, Hiroshima 734-8553, Japan.

出版信息

J Histochem Cytochem. 2002 Apr;50(4):483-92. doi: 10.1177/002215540205000405.

DOI:10.1177/002215540205000405
PMID:11897801
Abstract

STC1, a mammalian homologue of stanniocalcin (STC) which plays a major role in calcium/phosphate homeostasis in fish, has been recently isolated. We have characterized the spatiotemporal distribution of STC1 mRNA and protein during mouse embryonic development generally and osteogenesis specifically. Northern blotting analysis of whole embryos showed that STC1 mRNA is highly and differentially expressed during embryogenesis. By in situ hybridization, STC1 mRNA was detected early in mesenchymal condensations and was then found to be highly expressed in perichondrial cells, periosteal cells, and then osteoblasts during endochondral bone formation. In bones forming by intramembranous ossification, STC1 mRNA was not detected until osteogenic cells appeared. The cellular distribution of STC1 protein closely corresponded to that of its mRNA, but the protein was also detected in hypertrophic chondrocytes. In the MC3T3-E1 osteogenic cell model, STC1 protein and mRNA were detectable throughout proliferation and differentiation stages but levels were relatively higher late during nodule formation/mineralization phases. For comparison, STC1 mRNA was also found in epithelial cells of both embryonic and adult intestine that had not previously been described among tissues responsive to calcium/phosphate transport. These results suggest that STC1 is expressed in a time- and cell-specific manner and may play an autocrine/paracrine role during osteoblast development and bone formation.

摘要

STC1是鱼类中在钙/磷稳态中起主要作用的鲽鱼降钙素(STC)的哺乳动物同源物,最近已被分离出来。我们已经描述了STC1 mRNA和蛋白在小鼠胚胎发育过程中的时空分布,特别是在骨生成过程中的分布。对整个胚胎的Northern印迹分析表明,STC1 mRNA在胚胎发育过程中高度且差异表达。通过原位杂交,在间充质凝聚早期检测到STC1 mRNA,然后发现在软骨内骨形成过程中,其在软骨膜细胞、骨膜细胞以及随后的成骨细胞中高度表达。在通过膜内成骨形成的骨骼中,直到成骨细胞出现才检测到STC1 mRNA。STC1蛋白的细胞分布与其mRNA的分布密切对应,但在肥大软骨细胞中也检测到了该蛋白。在MC3T3-E1成骨细胞模型中,在整个增殖和分化阶段都可检测到STC1蛋白和mRNA,但在结节形成/矿化阶段后期水平相对较高。作为比较,在胚胎和成年肠道的上皮细胞中也发现了STC1 mRNA,此前在对钙/磷转运有反应的组织中尚未描述过。这些结果表明,STC1以时间和细胞特异性方式表达,并且可能在成骨细胞发育和骨形成过程中发挥自分泌/旁分泌作用。

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