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衰老加速小鼠(SAMP6)的特定部位骨丢失:一种用于衰老性骨质疏松症的鼠模型。

Site-specific bone loss in senescence-accelerated mouse (SAMP6): a murine model for senile osteoporosis.

机构信息

Department of Anatomy, Gifu University Graduate School of Medicine, 1-1 Yanagido, Gifu 501-1194, Japan.

出版信息

Exp Gerontol. 2009 Dec;44(12):792-8. doi: 10.1016/j.exger.2009.09.009. Epub 2009 Oct 6.

Abstract

The senescence-accelerated mouse strain P6 (SAMP6) is a model of senile osteoporosis, which possesses many features of senile osteoporosis in humans. So far, little is known about the systemic bone microstructural changes that occur at multiple skeletal sites. In this study, we therefore, investigated site (vertebra, femur and tibia) dependence of bone microstructure and bone mineral density (BMD) in SAMP6 and the normal control mouse (SAMR1) at 5 and 12months of age using quantitative micro computed tomography (micro-CT) and image analysis software. As compared with SAMR1, the most prominent change in SAMP6 was the reduction of vertebral trabecular bone volume fraction (BV/TV) and trabecular BMD. Moderate decrease of trabecular bone mass was observed in the proximal tibia and distal femur. Increased marrow area and periosteal perimeter were investigated, though the cortical area and cortical thickness had no marked changes in the mid-tibial and mid-femoral cortical bones. These results indicate that bone microstructural properties in SAMP6 are remarkably heterogeneous throughout the skeleton, which is analogous to changes that occur in human bones. These findings further validate the relevance of SAMP6 as a model of senile osteoporosis.

摘要

衰老加速小鼠品系 P6(SAMP6)是一种衰老性骨质疏松模型,具有许多人类衰老性骨质疏松的特征。到目前为止,人们对发生在多个骨骼部位的系统性骨微观结构变化知之甚少。因此,本研究采用定量微计算机断层扫描(micro-CT)和图像分析软件,在 5 个月和 12 个月大时,研究了 SAMP6 和正常对照鼠(SAMR1)的骨骼部位(椎体、股骨和胫骨)依赖性骨微观结构和骨密度(BMD)。与 SAMR1 相比,SAMP6 最明显的变化是椎体小梁骨体积分数(BV/TV)和小梁骨密度的降低。在胫骨近端和股骨远端观察到中等程度的小梁骨量减少。研究了骨髓面积和骨膜周长的增加,尽管中胫骨和中股骨皮质骨的皮质面积和皮质厚度没有明显变化。这些结果表明,SAMP6 骨骼中的骨微观结构特性在整个骨骼中存在明显的异质性,这类似于人类骨骼中发生的变化。这些发现进一步验证了 SAMP6 作为衰老性骨质疏松模型的相关性。

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