OPN, BSP, and Bone Quality-Structural, Biochemical, and Biomechanical Assessment in OPN-/-, BSP-/-, and DKO Mice.

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2024-07-01 Epub Date: 2024-05-11 DOI:10.1007/s00223-024-01217-0
Luc Malaval, Hélène Follet, Delphine Farlay, Evelyne Gineyts, Sebastien Rizzo, Charlene Thomas, Mathieu Maalouf, Myriam Normand, Brigitte Burt-Pichat, Wafa Bouleftour, Arnaud Vanden-Boscche, Norbert Laroche, Laurence Vico
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Abstract

Osteopontin (OPN) and Bone Sialoprotein (BSP), abundantly expressed by osteoblasts and osteoclasts, appear to have important, partly overlapping functions in bone. In gene-knockout (KO, -/-) models of either protein and their double (D)KO in the same CD1/129sv genetic background, we analyzed the morphology, matrix characteristics, and biomechanical properties of femur bone in 2 and 4 month old, male and female mice. OPN-/- mice display inconsistent, perhaps localized hypermineralization, while the BSP-/- are hypomineralized throughout ages and sexes, and the low mineralization of young DKO mice recovers with age. The higher contribution of primary bone remnants in OPN-/- shafts suggests a slow turnover, while their lower percentage in BSP-/- indicates rapid remodeling, despite FTIR-based evidence in this genotype of a high maturity of the mineralized matrix. In 3-point bending assays, OPN-/- bones consistently display higher Maximal Load, Work to Max. Load and in young mice Ultimate Stress, an intrinsic characteristic of the matrix. Young male and old female BSP-/- also display high Work to Max. Load along with low Ultimate Stress. Principal Component Analysis confirms the major role of morphological traits in mechanical competence, and evidences a grouping of the WT phenotype with the OPN-/- and of BSP-/- with DKO, driven by both structural and matrix parameters, suggesting that the presence or absence of BSP has the most profound effects on skeletal properties. Single or double gene KO of OPN and BSP thus have multiple distinct effects on skeletal phenotypes, confirming their importance in bone biology and their interplay in its regulation.

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OPN、BSP 和骨质--OPN-/-、BSP-/- 和 DKO 小鼠的结构、生化和生物力学评估。
成骨细胞和破骨细胞大量表达的骨蛋白(OPN)和骨硅蛋白(BSP)似乎在骨骼中具有重要的、部分重叠的功能。在相同的 CD1/129sv 遗传背景下,我们对基因敲除(KO、-/-)两种蛋白的模型及其双(D)KO模型进行了研究,分析了 2 个月和 4 个月大的雄性和雌性小鼠股骨的形态、基质特征和生物力学特性。OPN-/- 小鼠表现出不一致的、可能是局部的高矿化,而 BSP-/- 在整个年龄段和性别都表现出低矿化,年轻 DKO 小鼠的低矿化随着年龄的增长而恢复。在 OPN-/- 轴中,原生骨残余物的比例较高,这表明骨转换速度较慢,而在 BSP-/- 中,原生骨残余物的比例较低,这表明骨重塑速度较快,尽管傅立叶变换红外光谱(FTIR)显示这种基因型的矿化基质成熟度较高。在三点弯曲试验中,OPN-/-骨骼始终显示出较高的最大载荷、最大工作载荷和年轻小鼠的极限载荷。在三点弯曲试验中,OPN-/-骨骼始终表现出较高的最大载荷、最大载荷至最大载荷的功以及年轻小鼠的极限应力,这是基质的固有特征。年轻雄性和老年雌性 BSP-/- 也显示出较高的最大载荷功和较低的极限应力。负载和低极限应力。主成分分析证实了形态学特征在机械能力中的主要作用,并证明了 WT 表型与 OPN-/- 和 BSP-/- 与 DKO 的分组,由结构和基质参数共同驱动,这表明 BSP 的存在与否对骨骼特性的影响最为深远。因此,OPN 和 BSP 的单基因或双基因 KO 对骨骼表型有多种不同的影响,证实了它们在骨生物学中的重要性及其在调控中的相互作用。
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7.20
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4.30%
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