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Versican splice variant messenger RNA expression in normal human Achilles tendon and tendinopathies.

机译:正常人的跟腱和腱病中的Versican剪接变体信使RNA表达。

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OBJECTIVES: Versican is the principal large proteoglycan expressed in mid-tendon, but its role in tendon pathology is unknown. Our objective was to define the expression of versican isoform splice variant messenger ribonucleic acid (mRNA) in normal Achilles tendons, in chronic painful tendinopathy and in ruptured tendons. METHODS: Total RNA isolated from frozen tendon samples (normal n = 14; chronic painful tendinopathy n = 10; ruptured n = 8) was assayed by relative quantitative reverse transcriptase polymerase chain reaction (RT-PCR) for total versican, versican variants V0, V1, V2, V3 and type I collagen alpha1 mRNA, normalized to glyceraldehyde-3-phosphate dehydrogenase (GAPDH). Differences between sample groups were tested by Wilcoxon statistics. RESULTS: Painful and ruptured tendons showed a significant decrease (median 2-fold) in the expression of versican mRNA, in contrast to an increased expression (median 8-fold) of type I collagen alpha1 mRNA in painful tendons. Versican splice variants V0 and V1 mRNA were readily detected in normal samples, V3 levels were substantially lower, and V2 levels were more variable. Each of V1, V2 and V3 mRNA showed significant decreases in expression in painful and ruptured tendons, but V0 was not significantly changed. CONCLUSIONS: Changes in versican expression relative to that of collagen, and alterations in the balance of versican splice variants, may contribute to changes in matrix structure and function in tendinopathies.
机译:目的:Versican是在肌腱中部表达的主要大蛋白聚糖,但在肌腱病理学中的作用尚不清楚。我们的目标是确定在正常的跟腱,慢性疼痛性肌腱病和断裂的肌腱中,versican亚型剪接变体信使核糖核酸(mRNA)的表达。方法:通过相对定量逆转录酶聚合酶链反应(RT-PCR)测定从冰冻肌腱样品(正常n = 14;慢性疼痛性肌腱病n = 10;破裂n = 8)中分离的总RNA,以检测总versican,versican变体V0, V1,V2,V3和I型胶原蛋白alpha1 mRNA,已标准化为3-磷酸甘油醛脱氢酶(GAPDH)。样本组之间的差异通过Wilcoxon统计进行检验。结果:疼痛和断裂的肌腱显示versican mRNA的表达显着减少(中位数2倍),而疼痛肌腱中I型胶原蛋白alpha1 mRNA的表达增加(中位数8倍)。在正常样品中很容易检测到Versican剪接变体V0和V1 mRNA,V3水平明显较低,而V2水平具有较大的可变性。 V1,V2和V3 mRNA在疼痛和断裂的肌腱中均显示出明显的降低,但V0没有明显改变。结论:versican表达相对于胶原蛋白的变化,以及versican剪接变体平衡的改变,可能有助于肌腱病变的基质结构和功能的变化。

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