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The bone morphogenetic protein antagonist Noggin is regulated by Sox9 during endochondral differentiation

机译:骨形态发生蛋白拮抗剂Noggin在软骨内分化过程中受Sox9调控

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摘要

Noggin has been described to be capable of binding bone morphogenetic proteins (BMP) and inhibiting BMP signaling by preventing the interactions of BMP with their receptors. Noggin expression during endochondral differentiation was analyzed to elucidate its potential role during chondrogenesis, Throughout mouse development, Noggin was expressed abundantly in the chondrocytic lineage as early as collagen type II RNA was detectable. In addition, a strong correlation was detected between Noggin expression and the expression profile of Sox9 during chondrogenesis. Sox9 (known to play an important role during chondrogenesis) and Noggin expression were investigated in the pluripotent mesenchymal cell line C3H10T1/2, stimulated by BMP-2. BMP-2 caused significant upregulation of Sox9 and Noggin expression in these cells. The upregulation of Noggin could be inhibited by introducing antisense oligonucleotides against Sox9 mRNA into the cells. Using mouse limb bud cultures, the role of Sox9 and Noggin during endochondral tissue differentiation was further studied, Treatment of cultures with Sox9 antisense oligonucleotides and/or Noggin protein caused significant alterations in limb morphogenesis and endochondral development. The data suggest that the transcriptional control of Noggin by Sox9 is a potent regulatory mechanism in chondrocyte differentiation.
机译:Noggin被描述为能够结合骨形态发生蛋白(BMP)并通过阻止BMP与它们的受体的相互作用来抑制BMP信号传导。分析了软骨内分化过程中的Noggin表达,以阐明其在软骨形成过程中的潜在作用。在小鼠的整个发育过程中,在可检测到II型胶原RNA的早期,Noggin就在软骨细胞谱系中大量表达。另外,在软骨形成过程中,在头蛋白表达和Sox9的表达谱之间检测到强相关性。在BMP-2刺激的多能间充质细胞系C3H10T1 / 2中研究了Sox9(在软骨形成过程中起着重要作用)和Noggin的表达。 BMP-2在这些细胞中引起Sox9和Noggin表达的显着上调。可以通过将针对Sox9 mRNA的反义寡核苷酸引入细胞来抑制Noggin的上调。使用小鼠肢芽培养物,进一步研究了Sox9和Noggin在软骨组织分化中的作用。用Sox9反义寡核苷酸和/或Noggin蛋白处理培养物会导致肢体形态发生和软骨内发育的显着改变。数据表明,Sox9对Noggin的转录控制是软骨细胞分化的有效调节机制。

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