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骨膜素基因敲除小鼠的骨膜骨形成随年龄变化。

Periosteal Bone Formation Varies with Age in Periostin Null Mice.

作者信息

Gardinier Joseph D, Chougule Amit, Mendez Devin, Daly-Seiler Conor, Zhang Chunbin

机构信息

Department of Orthopedics, Bone and Joint Center, Henry Ford Health System, 6135 Woodward Avenue, Detroit, MI, 48202, USA.

School of Medicine, Wayne State University, Detroit, MI, USA.

出版信息

Calcif Tissue Int. 2023 Apr;112(4):463-471. doi: 10.1007/s00223-023-01063-6. Epub 2023 Feb 2.

DOI:10.1007/s00223-023-01063-6
PMID:36729140
Abstract

Periostin, also known as osteoblast-specific factor 2, is a matricellular protein predominantly expressed at the periosteum of bone. During growth and development, periostin contributes to periosteal expansion by facilitating osteoblast differentiation and mineralization. Later in life, periosteal expansion provides an adaptive strategy to increase tissue strength without requiring substantial increase in bone mass. However, the function of periostin past skeletal maturity and during advanced aging is relatively unknown. The objective of this study was to examine the function of periostin in maintaining bone mass and tissue strength across different ages. In periostin null mice (Postn-/-), periosteal bone formation was significantly reduced in young (3 months) and adult mice (9 months). The lack of bone formation resulted in reduced bone mass and ultimate strength. Conversely, periosteal bone formation increased at advanced ages in 18-month-old Postn-/- mice. The increase in periosteal mineralization at advanced ages coincides with increased expression of vitronectin and osteopontin. Periosteal progenitors from Postn-/- mice displayed an increased capacity to mineralize when cultured on vitronectin, but not type-1 collagen. Altogether, these findings demonstrate the unique role of periostin in regulating periosteal bone formation at different ages and the potential for vitronectin to compensate in the absence of periostin.

摘要

骨膜蛋白,也被称为成骨细胞特异性因子2,是一种主要在骨膜表达的基质细胞蛋白。在生长发育过程中,骨膜蛋白通过促进成骨细胞分化和矿化来促进骨膜扩张。在生命后期,骨膜扩张提供了一种适应性策略,在不显著增加骨量的情况下增强组织强度。然而,骨膜蛋白在骨骼成熟后及衰老过程中的功能相对未知。本研究的目的是探讨骨膜蛋白在不同年龄维持骨量和组织强度中的作用。在骨膜蛋白基因敲除小鼠(Postn-/-)中,年轻(3个月)和成年小鼠(9个月)的骨膜骨形成显著减少。骨形成的缺乏导致骨量和极限强度降低。相反,18个月大的Postn-/-小鼠在老年时骨膜骨形成增加。老年时骨膜矿化的增加与玻连蛋白和骨桥蛋白表达的增加相一致。当在玻连蛋白而非I型胶原上培养时,来自Postn-/-小鼠的骨膜祖细胞矿化能力增强。总之,这些发现证明了骨膜蛋白在不同年龄调节骨膜骨形成中的独特作用,以及在缺乏骨膜蛋白时玻连蛋白的潜在补偿作用。

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本文引用的文献

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2
Bone adaptation in response to treadmill exercise in young and adult mice.幼年和成年小鼠对跑步机运动的骨骼适应性
Bone Rep. 2018 Jan 12;8:29-37. doi: 10.1016/j.bonr.2018.01.003. eCollection 2018 Jun.
3
A vitronectin-derived peptide reverses ovariectomy-induced bone loss via regulation of osteoblast and osteoclast differentiation.
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