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首页> 外文期刊>Journal of orthopaedic research >Gene expression changes in SNAP-stimulated and iNOS-transfected tenocytes--expression of extracellular matrix genes and its implications for tendon-healing.
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Gene expression changes in SNAP-stimulated and iNOS-transfected tenocytes--expression of extracellular matrix genes and its implications for tendon-healing.

机译:SNAP刺激和iNOS转染的肌腱细胞中的基因表达变化-细胞外基质基因的表达及其对腱愈合的影响。

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摘要

Nitric oxide (NO) has a variety of physiological roles, including acting as a key mediator in various phases of tendon healing, but its importance as a modulator of gene expression during tendon healing has not been well studied. The current study used microarray analysis to elucidate global gene expression after transfection with inducible nitric oxide synthase (iNOS) in tenocytes isolated from the injured rotator cuff tendons of human patients. We show that the expression of a wide range of genes is affected by NO, with many activated genes having known roles in healing. Of particular significance is that NOS overexpression stimulates the transcription and translation of a range of extracellular matrix genes important to the structure of connective tissues such as tendons, including collagen Ialpha1, collagen IIIalpha1, collagen IValpha5, biglycan, decorin, laminin, and matrix metalloproteinase 10 (MMP10). These genes were also shown to respond to stimulation by the NO donor S-nitroso-N-acetyl-penicillamine (SNAP) in a dose-dependent manner. We further show that varying levels of NO significantly affect cellular adhesion in tenocytes, a critical process during tendon repair. These findings will be of use when optimizing the dose of NO delivery in further work investigating NO as potential treatment of tendon injuries.
机译:一氧化氮(NO)具有多种生理作用,包括在肌腱愈合的各个阶段充当关键介体,但尚未很好地研究其在肌腱愈合过程中作为基因表达调节剂的重要性。目前的研究使用微阵列分析来阐明转染诱导型一氧化氮合酶(iNOS)从人患者受伤的肩袖肌腱分离的肌腱细胞中的整体基因表达。我们表明,广泛的基因表达受到NO的影响,许多活化的基因在愈合中具有已知作用。尤其重要的是,NOS的过度表达刺激了一系列结缔组织结构(如肌腱)的重要胞外基质基因的转录和翻译,这些结缔组织包括胶原蛋白Ialpha1,胶原蛋白IIIalpha1,胶原蛋白IValpha5,双糖聚糖,核心蛋白聚糖,层粘连蛋白和基质金属蛋白酶10 (MMP10)。这些基因还显示出以剂量依赖性方式对NO供体S-亚硝基-N-乙酰基-青霉胺(SNAP)的刺激反应。我们进一步表明,不同水平的NO会显着影响肌腱细胞的细胞粘附,这是肌腱修复过程中的关键过程。这些发现将在优化NO输送剂量以进一步研究NO作为肌腱损伤的潜在治疗方法时有用。

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