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在成年小鼠中,成骨细胞和内皮细胞中的Bmp2条件性敲除不会损害损伤或机械负荷后的骨形成。

Bmp2 conditional knockout in osteoblasts and endothelial cells does not impair bone formation after injury or mechanical loading in adult mice.

作者信息

McBride-Gagyi Sarah Howe, McKenzie Jennifer A, Buettmann Evan G, Gardner Michael J, Silva Matthew J

机构信息

Department of Orthopaedic Surgery, Saint Louis University School of Medicine, 1402 S. Grand Blvd, Schwitalla Hall, M176, St. Louis, MO 63104, USA; Department of Orthopedic Surgery, Washington University in St. Louis School of Medicine, 660 S. Euclid, Campus Box8233, St. Louis, MO 63110, USA.

Department of Orthopedic Surgery, Washington University in St. Louis School of Medicine, 660 S. Euclid, Campus Box8233, St. Louis, MO 63110, USA.

出版信息

Bone. 2015 Dec;81:533-543. doi: 10.1016/j.bone.2015.09.003. Epub 2015 Sep 5.

DOI:10.1016/j.bone.2015.09.003
PMID:26344756
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4640950/
Abstract

Post-natal osteogenesis after mechanical trauma or stimulus occurs through either endochondral healing, intramembranous healing or lamellar bone formation. Bone morphogenetic protein 2 (BMP2) is up-regulated in each of these osteogenic processes and is expressed by a variety of cells including osteoblasts and vascular cells. It is known that genetic knockout of Bmp2 in all cells or in osteo-chondroprogenitor cells completely abrogates endochondral healing after full fracture. However, the importance of BMP2 from differentiated osteoblasts and endothelial cells is not known. Moreover, the importance of BMP2 in non-endochondral bone formation such as intramembranous healing or lamellar bone formation is not known. Using inducible and tissue-specific Cre-lox mediated targeting of Bmp2 in adult (10-24 week old) mice, we assessed the role of BMP2 expression globally, by osteoblasts, and by vascular endothelial cells in endochondral healing, intramembranous healing and lamellar bone formation. These three osteogenic processes were modeled using full femur fracture, ulnar stress fracture, and ulnar non-damaging cyclic loading, respectively. Our results confirmed the requirement of BMP2 for endochondral fracture healing, as mice in which Bmp2 was knocked out in all cells prior to fracture failed to form a callus. Targeted deletion of Bmp2 in osteoblasts (osterix-expressing) or vascular endothelial cells (vascular endothelial cadherin-expressing) did not impact fracture healing in any way. Regarding non-endochondral bone formation, we found that BMP2 is largely dispensable for intramembranous bone formation after stress fracture and also not required for lamellar bone formation induced by mechanical loading. Taken together our results indicate that osteoblasts and endothelial cells are not a critical source of BMP2 in endochondral fracture healing, and that non-endochondral bone formation in the adult mouse is not as critically dependent on BMP2.

摘要

机械创伤或刺激后的产后骨生成通过软骨内愈合、膜内愈合或板层骨形成实现。骨形态发生蛋白2(BMP2)在这些成骨过程中均上调,并由包括成骨细胞和血管细胞在内的多种细胞表达。已知在所有细胞或骨软骨祖细胞中敲除Bmp2基因会完全消除完全骨折后的软骨内愈合。然而,来自分化的成骨细胞和内皮细胞的BMP2的重要性尚不清楚。此外,BMP2在非软骨内骨形成(如膜内愈合或板层骨形成)中的重要性也不清楚。利用诱导性和组织特异性Cre-lox介导的成年(10-24周龄)小鼠Bmp2靶向,我们评估了BMP2在软骨内愈合、膜内愈合和板层骨形成中整体、由成骨细胞以及由血管内皮细胞表达的作用。分别使用全股骨骨折、尺骨应力性骨折和尺骨无损伤循环负荷对这三种成骨过程进行建模。我们的结果证实了软骨内骨折愈合需要BMP2,因为在骨折前所有细胞中敲除Bmp2的小鼠未能形成骨痂。在成骨细胞(表达osterix)或血管内皮细胞(表达血管内皮钙黏蛋白)中靶向缺失Bmp2对骨折愈合没有任何影响。关于非软骨内骨形成,我们发现BMP2在应力性骨折后的膜内骨形成中基本 dispensable,在机械负荷诱导的板层骨形成中也不需要。综上所述,我们的结果表明,成骨细胞和内皮细胞不是软骨内骨折愈合中BMP2的关键来源,并且成年小鼠的非软骨内骨形成对BMP2的依赖性没有那么关键。 (注:原文中“dispensable”未翻译完整,可能是有遗漏信息,正常意思是“可有可无的、非必需的” )

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