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首页> 外文期刊>Cell biology international. >RNA interference of the BMPR-IB gene blocks BMP-2-induced osteogenic gene expression in human bone cells.
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RNA interference of the BMPR-IB gene blocks BMP-2-induced osteogenic gene expression in human bone cells.

机译:BMPR-IB基因的RNA干扰会阻止BMP-2诱导的人骨细胞中成骨基因表达。

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We have previously shown that human bone cells express bone morphogenetic protein receptor-IB (BMPR-IB). However, little is known about the precise role of this receptor in the response of osteoblastic genes to the BMP in these cells. To determine BMPR-IB-dependent osteoblastic gene expression, the present study examined the effects of BMPR-IB knockdown on BMP-induced osteoblast-associated genes. BMPR-IB mRNA and protein were markedly suppressed by transfection of cells with BMPR-IB siRNA. Using three different bone cell samples, BMP-2 stimulation of alkaline phosphatase (ALP), osteocalcin (OC), distal-less homeobox-5 (Dlx5) and core binding factor alpha-1 (Cbfa1) was found to be specifically and significantly reduced in the BMPR-IB siRNA-transfected cultures compared with that of control cultures. Our study has provided evidence that BMPR-IB-dependent signaling plays a crucial role in BMP-2 up-regulation of the ALP, OC, Dlx5 and Cbfa1 genes in bone cells, suggesting a pivotal role of this receptor in BMP-2-induced osteoblast differentiation in vitro. These findings thus suggest the possibility that BMPR-IB could be a therapeutic target for enhancing bone regeneration in vivo.
机译:先前我们已经表明,人的骨细胞表达骨形态发生蛋白受体-IB(BMPR-IB)。但是,关于这种受体在这些细胞中成骨细胞基因对BMP的反应中的确切作用了解甚少。为了确定BMPR-IB依赖的成骨细胞基因表达,本研究检查了BMPR-IB敲低对BMP诱导的成骨细胞相关基因的影响。通过用BMPR-IB siRNA转染细胞,可以显着抑制BMPR-IB mRNA和蛋白质。使用三种不同的骨细胞样本,发现BMP-2对碱性磷酸酶(ALP),骨钙素(OC),远侧无源Homeobox-5(Dlx5)和核心结合因子α-1(Cbfa1)的刺激显着降低与对照培养相比,在BMPR-IB siRNA转染的培养物中的表达水平升高。我们的研究提供了证据,表明BMPR-IB依赖性信号传导在骨细胞中ALP,OC,Dlx5和Cbfa1基因的BMP-2上调中起关键作用,表明该受体在BMP-2诱导中起关键作用体外成骨细胞分化。这些发现因此暗示了BMPR-1B可能是用于增强体内骨再生的治疗靶标的可能性。

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