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成骨细胞中转录因子Runx2的过表达消除了甲状旁腺激素在体内的合成代谢作用。

Overexpression of the transcriptional factor Runx2 in osteoblasts abolishes the anabolic effect of parathyroid hormone in vivo.

作者信息

Merciris Didier, Marty Caroline, Collet Corinne, de Vernejoul Marie-Christine, Geoffroy Valerie

机构信息

INSERM U606, University Paris 7, Paris, France.

出版信息

Am J Pathol. 2007 May;170(5):1676-85. doi: 10.2353/ajpath.2007.061069.

DOI:10.2353/ajpath.2007.061069
PMID:17456773
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1854962/
Abstract

There is convincing evidence that Runx2 could be a regulator of the anabolic action of parathyroid hormone (PTH) in bone. We therefore decided to determine how Runx2 overexpression in osteoblasts affects the anabolic response to PTH. Transgenic osteoporotic female mice overexpressing Runx2 (TG) and their wild-type littermates (WT) were treated with PTH (100 microg/kg/day, 7 days a week) or with the vehicle for 6 weeks. Unexpectedly, Runx2 overexpression blunted the increase in the mineral density and volume of bone induced by intermittent PTH in WT mice. Our findings also indicate that PTH failed to increase bone formation in TG mice overexpressing Runx2. This abolition of the effect of PTH by Runx2 overexpression was attributable to a decrease in the differentiation of osteoblastic cells both in vivo and in vitro. Finally, we showed that less cAMP was induced by PTH and that there were fewer PTH binding sites in TG than WT osteoblasts. In conclusion, our findings demonstrate that in vivo a high level of Runx2 abolishes the anabolic effect of PTH, probably via a decrease in the sensitivity of TG osteoblasts to PTH, and that the level of expression of Runx2 is critical if PTH is to produce its anabolic effect on bone in vivo.

摘要

有令人信服的证据表明,Runx2可能是甲状旁腺激素(PTH)在骨骼中合成代谢作用的调节因子。因此,我们决定确定成骨细胞中Runx2过表达如何影响对PTH的合成代谢反应。对过表达Runx2的转基因骨质疏松雌性小鼠(TG)及其野生型同窝小鼠(WT)给予PTH(100微克/千克/天,每周7天)或赋形剂处理6周。出乎意料的是,Runx2过表达减弱了WT小鼠中由间歇性PTH诱导的骨矿物质密度和骨体积的增加。我们的研究结果还表明,PTH未能增加过表达Runx2的TG小鼠的骨形成。Runx2过表达导致PTH效应的消除归因于体内和体外成骨细胞分化的减少。最后,我们发现PTH诱导产生的cAMP较少,并且TG成骨细胞中的PTH结合位点比WT成骨细胞中的少。总之,我们的研究结果表明,在体内高水平的Runx2消除了PTH的合成代谢作用,可能是通过降低TG成骨细胞对PTH的敏感性,并且如果PTH要在体内对骨骼产生合成代谢作用,Runx2的表达水平至关重要。

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