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Vertebral endplate architecture and vascularization: application of micro-computerized tomography, a vascular tracer, and immunocytochemistry in analyses of disc degeneration in the aging sand rat.

机译:椎终板结构和血管化:微计算机断层扫描,血管示踪剂和免疫细胞化学在老化沙鼠椎间盘退变分析中的应用。

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STUDY DESIGN: Lower lumbar vertebral endplates from young and old sand rats were assessed in an Institutional Animal Care and Use Committee approved study for architectural endplate features using micro-computerized tomography (CT) 3-dimensional (3D) models and vascularization studies by an in vivo vascular tracer or immunocytochemical identification of blood vessels. OBJECTIVE: To assess endplate porosity and vascularization using microCT architectural analysis, an in vivo vascular tracer, and immunocytochemical identification of blood vessels in the endplate. SUMMARY OF THE BACKGROUND DATA: The vertebral endplates, also called cartilage endplates, form the superior and inferior, or cranial and caudal, boundaries of the disc. In the human being and sand rat, the cartilaginous endplate undergoes calcification with aging and is replaced by bone. Endplate sclerosis has long been thought to play a role in disc degeneration by decreasing nutrient availability to the disc, but this is still poorly understood. Previous work has identified increasing bone mineral density with aging and disc degeneration in the sand rat model. METHODS: microCT models of the lower lumbar endplates of vertebrae at L5-6 and L6-7 were constructed from 6 younger (mean age 11 months) and 21 older (mean age 25.6 months) sand rats. Architectural features were scored on a semiquantitative scale for smoothness of the endplate face, irregularities on the endplate margin, and endplate thickness. There were 2 smaller sets of animals (n = 18) evaluated for endplate vascularity following in vivo injection of a fluorescent vascular tracer or by the use of immunocytochemistry to identify blood vessels. RESULTS: microCT revealed a solid bony surface to the endplate, which was not penetrated by vasculature; with aging/disc degeneration, there was roughening and pitting of the plate surface, and the development of irregular margins. In L5-6 and L6-7, sites of prominent disc degeneration evident on radiographs, the proportion of abnormalities in surface smoothness, margin irregularity, and endplate thickening were all statistically significant in both younger and older animals (P < or = 0.0027). More severe changes were evident in the caudal versus cranial endplate surfaces. Histologic study of vascular tracer showed that there was no penetration of the disc by vascular supply from the endplate; this was verified by immunocytochemical identification of blood vessels. The canal system within the endplate was a complex 3D interconnected network. CONCLUSIONS: Findings show that disc degeneration in the sand rat occurs concomitantly with marked architectural bony changes on the endplate face, including loss of smoothness and development of irregular bony margins. Vascular connections were not present between the endplate and disc; this was verified with microCT studies, in vivo vascular tracers, and traditional immunocytochemistry. The canal system within the imaged endplate was revealed to consist of a complex 3D interconnected network.
机译:研究设计:在由机构动物护理和使用委员会批准的一项关于建筑终板特征的研究中,使用了微型计算机断层扫描(CT)3维(3D)模型和一个血管形成研究,对年轻和老年沙鼠的下腰椎终板进行了评估。体内血管示踪或血管免疫细胞化学鉴定。目的:使用microCT架构分析,体内血管示踪剂和终板血管的免疫细胞化学鉴定,评估终板的孔隙率和血管形成。背景技术概述:椎骨终板,也称为软骨终板,形成了椎间盘的上,下,或颅和尾的边界。在人类和沙鼠中,软骨终板会随着年龄的增长而钙化,并被骨头取代。长期以来,人们一直认为终板硬化症通过减少椎间盘的养分利用率而在椎间盘退变中发挥作用,但对此知之甚少。先前的工作已经确定,沙鼠模型中的骨矿物质密度会随着老化和椎间盘退变而增加。方法:采用6只年轻(平均年龄11个月)和21只较大(平均年龄25.6个月)沙鼠建立L5-6和L6-7椎骨下腰椎终板的microCT模型。对建筑特征进行半定量评分,以评估端板表面的光滑度,端板边缘的不规则度和端板厚度。在体内注射荧光血管示踪剂或使用免疫细胞化学鉴定血管后,评估了2组较小的动物(n = 18)的终板血管性。结果:microCT显示终板有坚硬的骨表面,没有被脉管系统穿透。随着老化/光盘变性,板表面出现粗糙和点蚀,边缘出现不规则现象。在L5-6和L6-7中,X射线照片上明显的椎间盘退变部位,幼年和年长动物的表面光滑度,边缘不规则性和终板增厚异常的比例均具有统计学意义(P <或= 0.0027)。尾端和颅端板表面的变化更为明显。血管示踪剂的组织学研究表明,终板的血管供应没有使椎间盘穿透。血管的免疫细胞化学鉴定证实了这一点。终板内的运河系统是一个复杂的3D互连网络。结论:研究结果表明,砂鼠的椎间盘退变同时伴随着终板表面明显的建筑骨改变,包括光滑度的丧失和不规则的骨切缘的发展。终板和椎间盘之间不存在血管连接。这已经通过microCT研究,体内血管示踪剂和传统的免疫细胞化学方法得到了验证。成像的端板上的运河系统显示出由复杂的3D互连网络组成。

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