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首页> 外文期刊>Spine >A new in vivo animal model to create intervertebral disc degeneration characterized by MRI, radiography, CT/discogram, biochemistry, and histology.
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A new in vivo animal model to create intervertebral disc degeneration characterized by MRI, radiography, CT/discogram, biochemistry, and histology.

机译:一种新的体内动物模型,可产生椎间盘退变,其特征在于MRI,放射线照相,CT / Discogram,生物化学和组织学。

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STUDY DESIGN: A new in vivo sheep model was developed that produced disc degeneration through the injection of 5-bromodeoxyuridine (BrdU) into the intervertebral disc. This process was studied using magnetic resonance imaging (MRI), radiography, CT/discogram, histology, and biochemistry. OBJECTIVES: To develop a sheep model of intervertebral disc degeneration that more faithfully mimics the pathologic hallmarks of human intervertebral disc degeneration. SUMMARY OF BACKGROUND DATA: Recent studies have shown age-related alterations in proteoglycan structure and organization in human intervertebral discs. An animal model that involves the use of age-related changes in disc cells can be beneficial over other more invasive degenerative models that involves directly damaging the matrix of disc tissue. METHODS: Twelve sheep were injected with BrdU or vehicle (phosphate-buffered saline) into the central region of separate lumbar discs. Intact discs were used as controls. At the 2-, 6-, 10-, and 14-week time points, discs underwent MRI, radiography, histology, and biochemical analyses. A CT/discogram study was performed at the 14-week time point. RESULTS: MRI demonstrated a progressive loss of T2-weighted signal intensity at BrdU-injected discs over the 14-week study period. Radiograph findings included osteophyte and disc space narrowing formed by 10 weeks post-BrdU treatment. CT discography demonstrated internal disc disruption in several BrdU-treated discs at the 14-week time point. Histology showed a progressive loss of the normal architecture and cell density of discs from the 2-week time point to the 14-week time point. A progressive loss of cell proliferation capacity, water content, and proteoglycans was also documented. CONCLUSIONS: BrdU injection into the central region of sheep discs resulted in degeneration of intervertebral discs. This progressive, degenerative process was confirmed using MRI, histology, and by observing changes in biochemistry. Degeneration occurred in a manner that was similar to that observed in human disc degeneration.
机译:研究设计:开发了一种新的体内绵羊模型,该模型通过将5-溴脱氧尿苷(BrdU)注入椎间盘而引起椎间盘退变。使用磁共振成像(MRI),放射线照相,CT / Discogram,组织学和生物化学研究了该过程。目的:建立绵羊椎间盘退变的模型,更忠实地模拟人椎间盘退变的病理学特征。背景数据摘要:最近的研究表明,人类椎间盘中蛋白聚糖的结构和组织与年龄有关。涉及使用椎间盘细胞中与年龄相关的变化的动物模型可能比涉及直接破坏椎间盘组织基质的其他更具侵入性的退化模型更为有益。方法:向十二只绵羊分别注射BrdU或溶媒(磷酸盐缓冲盐水)到单独的腰间盘中央区域。完整的光盘用作对照。在第2、6、10和14周的时间点,对椎间盘进行MRI,放射线照相,组织学和生化分析。在14周的时间点进行了CT / Discogram研究。结果:MRI证实在14周的研究期间,BrdU注射椎间盘的T2加权信号强度逐渐丧失。 X射线照片包括BrdU治疗10周后形成的骨赘和椎间盘狭窄。 CT盘片显示在14周的时间点,数个BrdU处理过的盘片内部盘片破裂。组织学显示从2周的时间点到14周的时间点,椎间盘的正常结构和细胞密度逐渐丧失。还记录了细胞增殖能力,水含量和蛋白聚糖的逐渐丧失。结论:将BrdU注射到绵羊椎间盘的中部导致椎间盘退变。通过核磁共振成像,组织学和观察生物化学变化,证实了这种渐进的变性过程。变性发生的方式与人类椎间盘变性中观察到的方式相似。

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