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核心蛋白聚糖对小鼠髌腱力学、成分和结构特性的影响。

Influence of decorin on the mechanical, compositional, and structural properties of the mouse patellar tendon.

作者信息

Dourte LeAnn M, Pathmanathan Lydia, Jawad Abbas F, Iozzo Renato V, Mienaltowski Michael J, Birk David E, Soslowsky Louis J

机构信息

McKay Orthopaedic Research Laboratory, University of Pennsylvania, Philadelphia, PA 19104-6081, USA.

出版信息

J Biomech Eng. 2012 Mar;134(3):031005. doi: 10.1115/1.4006200.

Abstract

The interactions of small leucine-rich proteoglycans (SLRPs) with collagen fibrils, their association with water, and their role in fibrillogenesis suggests that SLRPs may play an important role in tendon mechanics. Some studies have assessed the role of SLRPs in the mechanical response of the tendon, but the relationships between sophisticated mechanics, assembly of collagen, and SLRPs have not been well characterized. Decorin content was varied in a dose dependent manner using decorin null, decorin heterozygote, and wild type mice. Quantitative measures of mechanical (tension and compression), compositional, and structural changes of the mouse patellar tendon were evaluated. Viscoelastic, tensile dynamic modulus was increased in the decorin heterozygous tendons compared to wild type. These tendons also had a significant decrease in total collagen and no structural changes compared to wild type. Decorin null tendons did not have any mechanical changes; however, a significant decrease in the average fibril diameter was found. No differences were seen between genotypes in elastic or compressive properties, and all tendons demonstrated viscoelastic mechanical dependence on strain rate and frequency. These results suggest that decorin, a member of the SLRP family, plays a role in tendon viscoelasticity that cannot be completely explained by its role in collagen fibrillogenesis. In addition, reductions in decorin do not cause large changes in indentation compressive properties, suggesting that other factors contribute to these properties. Understanding these relationships may ultimately help guide development of tissue engineered constructs or treatment modalities.

摘要

富含亮氨酸的小分子蛋白聚糖(SLRPs)与胶原纤维的相互作用、它们与水的结合以及它们在纤维形成中的作用表明,SLRPs可能在肌腱力学中发挥重要作用。一些研究评估了SLRPs在肌腱力学反应中的作用,但复杂力学、胶原组装和SLRPs之间的关系尚未得到充分表征。使用核心蛋白聚糖基因敲除小鼠、核心蛋白聚糖杂合子小鼠和野生型小鼠,以剂量依赖方式改变核心蛋白聚糖含量。对小鼠髌腱的力学(拉伸和压缩)、成分和结构变化进行了定量测量。与野生型相比,核心蛋白聚糖杂合子肌腱的粘弹性拉伸动态模量增加。与野生型相比,这些肌腱的总胶原含量也显著降低,且无结构变化。核心蛋白聚糖基因敲除的肌腱没有任何力学变化;然而,发现平均纤维直径显著减小。在弹性或压缩特性方面,各基因型之间未见差异,所有肌腱均表现出粘弹性力学对应变率和频率的依赖性。这些结果表明,核心蛋白聚糖作为SLRP家族的一员,在肌腱粘弹性中发挥作用,而这不能完全由其在胶原纤维形成中的作用来解释。此外,核心蛋白聚糖的减少不会导致压痕压缩特性的大幅变化,这表明其他因素也有助于这些特性。了解这些关系最终可能有助于指导组织工程构建体的开发或治疗方式。

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