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鉴定透明质酸增强软骨形成的潜在生物物理和分子信号机制。

Identification of potential biophysical and molecular signalling mechanisms underlying hyaluronic acid enhancement of cartilage formation.

机构信息

Department of Bioengineering, Rice University, , 6500 Main St., Suite 135, Houston, TX 77030, USA.

出版信息

J R Soc Interface. 2012 Dec 7;9(77):3564-73. doi: 10.1098/rsif.2012.0399. Epub 2012 Jul 18.

Abstract

This study determined the effects of exogenous hyaluronic acid (HA) on the biomechanical and biochemical properties of self-assembled bovine chondrocytes, and investigated biophysical and genetic mechanisms underlying these effects. The effects of HA commencement time, concentration, application duration and molecular weight were examined using histology, biomechanics and biochemistry. Additionally, the effects of HA application on sulphated glycosaminoglycan (GAG) retention were assessed. To investigate the influence of HA on gene expression, microarray analysis was conducted. HA treatment of developing neocartilage increased compressive stiffness onefold and increased sulphated GAG content by 35 per cent. These effects were dependent on HA molecular weight, concentration and application commencement time. Additionally, applying HA increased sulphated GAG retention within self-assembled neotissue. HA administration also upregulated 503 genes, including multiple genes associated with TGF-β1 signalling. Increased sulphated GAG retention indicated that HA could enhance compressive stiffness by increasing the osmotic pressure that negatively charged GAGs create. The gene expression data demonstrate that HA treatment differentially regulates genes related to TGF-β1 signalling, revealing a potential mechanism for altering matrix composition. These results illustrate the potential use of HA to improve cartilage regeneration efforts and better understand cartilage development.

摘要

本研究旨在确定外源性透明质酸(HA)对自组装牛软骨细胞生物力学和生化特性的影响,并探讨其潜在的生物物理和遗传机制。通过组织学、生物力学和生物化学方法研究了 HA 起始时间、浓度、作用时间和分子量的影响。此外,还评估了 HA 对硫酸化糖胺聚糖(GAG)保留的影响。为了研究 HA 对基因表达的影响,进行了微阵列分析。HA 处理发育中的新软骨可使压缩刚度增加一倍,并使硫酸化 GAG 含量增加 35%。这些作用依赖于 HA 的分子量、浓度和起始作用时间。此外,施加 HA 可增加新组织内硫酸化 GAG 的保留。HA 给药还上调了 503 个基因,包括多个与 TGF-β1 信号转导相关的基因。硫酸化 GAG 保留的增加表明,HA 可以通过增加带负电荷的 GAG 产生的渗透压来提高压缩刚度。基因表达数据表明,HA 处理可差异调节与 TGF-β1 信号转导相关的基因,揭示了改变基质组成的潜在机制。这些结果表明,HA 具有改善软骨再生的潜力,并有助于更好地理解软骨发育。

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