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唑来膦酸作用下,骨髓成骨前体细胞耗竭,而破骨细胞则在成骨血管之外被独立扩增。

Bone marrow osteoprogenitors are depleted whereas osteoblasts are expanded independent of the osteogenic vasculature in response to zoledronic acid.

机构信息

Department of Oncology and Metabolism, Experimental Cancer Medicine Centre, University of Sheffield, Sheffield, United Kingdom.

Department of Physics and Astronomy, University of Sheffield, Sheffield, United Kingdom.

出版信息

FASEB J. 2019 Nov;33(11):12768-12779. doi: 10.1096/fj.201900553RR. Epub 2019 Sep 6.

Abstract

Zoledronic acid (ZOL) is an antiresorptive drug used to prevent bone loss in a variety of conditions, acting mainly through suppression of osteoclast activity. There is growing evidence that ZOL can also affect cells of the mesenchymal lineage in bone. We present novel data revealing significant changes in the abundance of perivascular mesenchymal stromal cells (MSCs)/osteoprogenitors and osteoblasts following the injection of ZOL, . In young mice with high bone turnover and an abundance of perivascular osteoprogenitors, ZOL significantly ( < 0.0001) increased new bone formation. This was accompanied by a decline in osterix-positive osteoprogenitors and a corresponding increase in osteoblasts. However, these effects were not observed in mature mice with low bone turnover. Interestingly, the ZOL-induced changes in cells of the mesenchymal lineage occurred independently of effects on the osteogenic vasculature. Thus, we demonstrate that a single, clinically relevant dose of ZOL can induce new bone formation in microenvironments enriched for perivascular MSC/osteoprogenitors and high osteogenic potential. This arises from the differentiation of perivascular osterix-positive MSC/osteoprogenitors into osteoblasts at sites that are innately osteogenic. Collectively, our data demonstrate that ZOL affects multiple cell types in bone and has differential effects depending on the level of bone turnover.-Hughes, R., Chen, X., Hunter, K. D., Hobbs, J. K., Holen, I., Brown, N. J. Bone marrow osteoprogenitors are depleted whereas osteoblasts are expanded independent of the osteogenic vasculature in response to zoledronic acid.

摘要

唑来膦酸(ZOL)是一种抗吸收药物,用于预防多种情况下的骨质流失,主要通过抑制破骨细胞活性发挥作用。越来越多的证据表明,ZOL 还可以影响骨骼中的间充质谱系细胞。我们提出了新的数据,揭示了 ZOL 注射后血管周间充质基质细胞(MSCs)/成骨前体细胞和成骨细胞丰度的显著变化,。在高骨转换和丰富的血管周成骨前体细胞的年轻小鼠中,ZOL 显著(<0.0001)增加了新骨形成。这伴随着osterix 阳性成骨前体细胞的减少和成骨细胞的相应增加。然而,这些作用在低骨转换的成熟小鼠中没有观察到。有趣的是,ZOL 对间充质谱系细胞的影响独立于对成骨血管的影响。因此,我们证明单次临床相关剂量的 ZOL 可以在富含血管周 MSC/成骨前体细胞和高成骨潜能的微环境中诱导新骨形成。这是由于血管周 osterix 阳性 MSC/成骨前体细胞在固有成骨部位分化为成骨细胞所致。总的来说,我们的数据表明 ZOL 影响骨骼中的多种细胞类型,并根据骨转换水平产生不同的作用。-休斯,R.,陈,X.,亨特,K. D.,霍布斯,J. K.,霍伦,I.,布朗,N. J. 骨髓成骨前体细胞耗竭,而成骨细胞在骨形成的血管之外响应唑来膦酸而扩张,独立于骨形成的血管。

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