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首页> 外文期刊>Journal of orthopaedic research >In vivo remodeling of intervertebral discs in response to short- and long-term dynamic compression.
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In vivo remodeling of intervertebral discs in response to short- and long-term dynamic compression.

机译:椎间盘的体内重塑,响应短期和长期动态压缩。

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摘要

This study evaluated how dynamic compression induced changes in gene expression, tissue composition, and structural properties of the intervertebral disc using a rat tail model. We hypothesized that daily exposure to dynamic compression for short durations would result in anabolic remodeling with increased matrix protein expression and proteoglycan content, and that increased daily load exposure time and experiment duration would retain these changes but also accumulate changes representative of mild degeneration. Sprague-Dawley rats (n = 100) were instrumented with an Ilizarov-type device and divided into three dynamic compression (2 week-1.5 h/day, 2 week-8 h/day, 8 week-8 h/day at 1 MPa and 1 Hz) and two sham (2 week, 8 week) groups. Dynamic compression resulted in anabolic remodeling with increased matrix mRNA expression, minimal changes in catabolic genes or disc structure and stiffness, and increased glysosaminoglycans (GAG) content in the nucleus pulposus. Some accumulation of mild degeneration with 8 week-8 h included loss of annulus fibrosus GAG and disc height although 8-week shams also had loss of disc height, water content, and minor structural alterations. We conclude that dynamic compression is consistent with a notion of healthy substantially disrupting disc structural integrity. A slow accumulation of changes similar to human disc degeneration occurred when dynamic compression was applied for excessive durations, but this degenerative shift was mild when compared to static compression, bending, or other interventions that create greater structural disruption.
机译:这项研究使用大鼠尾巴模型评估了动态压缩如何诱导基因表达,组织组成和椎间盘结构特性的变化。我们假设每日短时间动态压缩会导致合成代谢重塑,增加基质蛋白表达和蛋白聚糖含量,而每天增加负荷暴露时间和实验持续时间会保留这些变化,但也会累积代表轻度变性的变化。用Ilizarov型器械对Sprague-Dawley大鼠(n = 100)进行器械测试,并将其分为三组动态压缩(在1 MPa下进行2周至1.5 h /天,2周至8 h /天,8周至8 h /天)和1 Hz)和两个假(2周,8周)组。动态压缩导致合成代谢重塑,其中基质mRNA表达增加,分解代谢基因或椎间盘结构和刚度的最小变化以及髓核中糖胺聚糖(GAG)含量增加。在8周至8 h时,轻度变性的一些累积包括纤维环GAG的丧失和椎间盘高度的损失,尽管8周的ms鼠也具有椎间盘高度,水分含量和较小的结构改变的损失。我们得出的结论是,动态压缩与健康破坏椎间盘结构完整性的概念一致。当施加动态压缩的持续时间过长时,会发生类似于人椎间盘退变的缓慢累积变化,但是与静态压缩,弯曲或其他会产生更大结构破坏的干预相比,该退行性变化较小。

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