首页> 外文期刊>International Journal of Experimental Pathology >Changes in calsequestrin, TNF-alpha, TGF-beta and MyoD levels during the progression of skeletal muscle dystrophy in mdx mice: a comparative analysis of the quadriceps, diaphragm and intrinsic laryngeal muscles
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Changes in calsequestrin, TNF-alpha, TGF-beta and MyoD levels during the progression of skeletal muscle dystrophy in mdx mice: a comparative analysis of the quadriceps, diaphragm and intrinsic laryngeal muscles

机译:mdx小鼠骨骼肌营养不良进展过程中钙螯合蛋白,TNF-α,TGF-β和MyoD水平的变化:股四头肌,diaphragm肌和喉固有肌的比较分析

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In Duchenne muscular dystrophy (DMD), the search for new biomarkers to follow the evolution of the disease is of fundamental importance in the light of the evolving gene and pharmacological therapies. In addition to the lack of dystrophin, secondary events including changes in calcium levels, inflammation and fibrosis greatly contribute to DMD progression and the molecules involved in these events may represent potential biomarkers. In this study, we performed a comparative evaluation of the progression of dystrophy within muscles that are differently affected by dystrophy (diaphragm; DIA and quadriceps; QDR) or spared (intrinsic laryngeal muscles) using the mdx mice model of DMD. We assessed muscle levels of calsequestrin (calcium-related protein), tumour necrosis factor (TNF-alpha; pro-inflammatory cytokine), tumour growth factor (TGF-beta; pro-fibrotic factor) and MyoD (muscle proliferation) vs. histopathology at early (1 and 4 months of age) and late (9 months of age) stages of dystrophy. Fibrosis was the primary feature in the DIA of mdx mice (9 months: 32% fibrosis), which was greater than in the QDR (9 months: 0.6% fibrosis). Muscle regeneration was the primary feature in the QDR (9 months: 90% of centrally nucleated fibres areas vs. 33% in the DIA). The QDR expressed higher levels of calsequestrin than the DIA. Laryngeal muscles showed normal levels of TNF-alpha, TGF-beta and MyoD. A positive correlation between histopathology and cytokine levels was observed only in the diaphragm, suggesting that TNF-alpha and TGF-beta serve as markers of dystrophy primarily for the diaphragm.
机译:在杜兴氏肌营养不良症(DMD)中,根据不断发展的基因和药物疗法,寻找新的生物标志物以追踪疾病的发展具有根本的重要性。除了缺乏肌营养不良蛋白外,包括钙水平变化,炎症和纤维化在内的继发性事件也极大地促进了DMD的发展,参与这些事件的分子可能代表了潜在的生物标志物。在这项研究中,我们使用DMD的mdx小鼠模型对受营养不良(横dia肌,DIA和股四头肌; QDR)或备用(喉内肌)不同影响的肌肉内营养不良的进展进行了比较评估。我们评估了Calsequestrin(钙相关蛋白),肿瘤坏死因子(TNF-α;促炎性细胞因子),肿瘤生长因子(TGF-beta;促纤维化因子)和MyoD(肌肉增生)与肌肉组织病理学水平的关系。营养不良的早期(1和4个月大)和晚期(9个月大)。纤维化是mdx小鼠DIA的主要特征(9个月:32%纤维化),大于QDR(9个月:0.6%纤维化)。肌肉再生是QDR的主要特征(9个月:中央有核纤维区域的90%,而DIA为33%)。 QDR表达的钙螯合蛋白水平高于DIA。喉肌显示正常水平的TNF-α,TGF-β和MyoD。仅在横diaphragm膜中观察到组织病理学与细胞因子水平之间呈正相关,这表明TNF-α和TGF-β主要是横the膜营养不良的标志物。

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