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Skeletal muscle tissue transcriptome differences in lean and obese female beagle dogs

机译:瘦和肥胖雌性比格犬的骨骼肌组织转录组差异

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Skeletal muscle is a large and insulin-sensitive tissue that is an important contributor to metabolic homeostasis and energy expenditure. Many metabolic processes are altered with obesity, but the contribution of muscle tissue in this regard is unclear. A limited number of studies have compared skeletal muscle gene expression of lean and obese dogs. Using microarray technology, our objective was to identify genes and functional classes differentially expressed in skeletal muscle of obese (14.6kg; 8.2 body condition score; 44.5% body fat) vs. lean (8.6kg; 4.1 body condition score; 22.9% body fat) female beagle adult dogs. Alterations in 77 transcripts was observed in genes pertaining to the functional classes of signaling, transport, protein catabolism and proteolysis, protein modification, development, transcription and apoptosis, cell cycle and differentiation. Genes differentially expressed in obese vs. lean dog skeletal muscle indicate oxidative stress and altered skeletal muscle cell differentiation. Many genes traditionally associated with lipid, protein and carbohydrate metabolism were not altered in obese vs. lean dogs, but genes pertaining to endocannabinoid metabolism, insulin signaling, type II diabetes mellitus and carnitine transport were differentially expressed. The relatively small response of skeletal muscle could indicate that changes are occurring at a post-transcriptional level, that other tissues (e.g., adipose tissue) were buffering skeletal muscle from metabolic dysfunction or that obesity-induced changes in skeletal muscle require a longer period of time and that the length of our study was not sufficient to detect them. Although only a limited number of differentially expressed genes were detected, these results highlight genes and functional classes that may be important in determining the etiology of obesity-induced derangement of skeletal muscle function.
机译:骨骼肌是一个大型且对胰岛素敏感的组织,是代谢稳态和能量消耗的重要因素。肥胖会改变许多新陈代谢过程,但是在这方面肌肉组织的作用尚不清楚。有限的研究比较了瘦狗和肥胖狗的骨骼肌基因表达。使用微阵列技术,我们的目标是鉴定肥胖(14.6kg; 8.2身体状况评分; 44.5%体脂)与瘦肉(8.6kg; 4.1身体状况评分; 22.9%体脂)在骨骼肌中差异表达的基因和功能类别)雌性小猎犬成年犬。在与信号传导,转运,蛋白质分解代谢和蛋白水解,蛋白质修饰,发育,转录和凋亡,细胞周期和分化的功能类别有关的基因中观察到77个转录物的改变。肥胖与瘦狗骨骼肌中差异表达的基因表明氧化应激和骨骼肌细胞分化改变。与肥胖,瘦狗相比,许多传统上与脂质,蛋白质和碳水化合物代谢相关的基因没有改变,但是与内源性大麻素代谢,胰岛素信号传导,II型糖尿病和肉碱运输有关的基因却有所差异。骨骼肌的响应相对较小,可能表明在转录后水平发生了变化,其他组织(例如脂肪组织)正在缓冲骨骼肌的代谢功能障碍,或者肥胖引起的骨骼肌变化需要更长的时间。时间,而且我们的研究时间不足以检测到它们。尽管仅检测到有限数量的差异表达基因,但这些结果突出了可能对确定肥胖引起的骨骼肌功能紊乱的病因重要的基因和功能类别。

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