Aerobic capacity and muscle proteome: Insights from a mouse model.

IF 2.6 4区 医学 Q2 PHYSIOLOGY Experimental Physiology Pub Date : 2024-11-21 DOI:10.1113/EP092308
Abel Plaza-Florido, Alejandro Santos-Lozano, Susana López-Ortiz, Beatriz G Gálvez, Joaquín Arenas, Miguel A Martín, Pedro L Valenzuela, Tomàs Pinós, Alejandro Lucia, Carmen Fiuza-Luces
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Abstract

We explored the association between aerobic capacity (AC) and the skeletal muscle proteome of McArdle (n = 10) and wild-type (n = 8) mice, as models of intrinsically 'low' and 'normal' AC, respectively. AC was determined as total distance achieved in treadmill running until exhaustion. The quadriceps muscle proteome was studied using liquid chromatography with tandem mass spectrometry, with the Search Tool for the Retrieval of Interacting Genes/Proteins database used to generate protein-protein interaction (PPI) networks and enrichment analyses. AC was significantly associated (P-values ranging from 0.0002 to 0.049) with 73 (McArdle) and 61 (wild-type) proteins (r-values from -0.90 to 0.94). These proteins were connected in PPI networks that enriched biological processes involved in skeletal muscle structure/function in both groups (false discovery rate <0.05). In McArdle mice, the proteins associated with AC were involved in skeletal muscle fibre differentiation/development, lipid oxidation, mitochondrial function and calcium homeostasis, whereas in wild-type animals AC-associated proteins were related to cytoskeleton structure (intermediate filaments), cell cycle regulation and endocytic trafficking. Two proteins (WEE2, THYG) were associated with AC (negatively and positively, respectively) in both groups. Only 14 of the 132 proteins (∼11%) associated with AC in McArdle or wild-type mice were also associated with those previously reported to be modified by aerobic training in these mice, providing preliminary evidence for a large divergence in the muscle proteome signature linked to aerobic training or AC, irrespective of AC (intrinsically low or normal) levels. Our findings might help to gain insight into the molecular mechanisms underlying AC at the muscle tissue level.

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有氧运动能力和肌肉蛋白质组:小鼠模型的启示
我们探讨了有氧运动能力(AC)与麦卡德尔小鼠(n = 10)和野生型小鼠(n = 8)骨骼肌蛋白质组之间的关系,这两种小鼠分别是有氧运动能力 "低 "和 "正常 "的模型。AC以跑步机上跑步至力竭的总距离来确定。使用液相色谱-串联质谱对股四头肌蛋白质组进行了研究,并使用检索相互作用基因/蛋白质的搜索工具数据库生成蛋白质-蛋白质相互作用(PPI)网络并进行富集分析。AC 与 73 个(McArdle)和 61 个(野生型)蛋白质(r 值在 -0.90 至 0.94 之间)有明显关联(P 值在 0.0002 至 0.049 之间)。这些蛋白质被连接到 PPI 网络中,该网络富集了两组中涉及骨骼肌结构/功能的生物过程(假发现率
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来源期刊
Experimental Physiology
Experimental Physiology 医学-生理学
CiteScore
5.10
自引率
3.70%
发文量
262
审稿时长
1 months
期刊介绍: Experimental Physiology publishes research papers that report novel insights into homeostatic and adaptive responses in health, as well as those that further our understanding of pathophysiological mechanisms in disease. We encourage papers that embrace the journal’s orientation of translation and integration, including studies of the adaptive responses to exercise, acute and chronic environmental stressors, growth and aging, and diseases where integrative homeostatic mechanisms play a key role in the response to and evolution of the disease process. Examples of such diseases include hypertension, heart failure, hypoxic lung disease, endocrine and neurological disorders. We are also keen to publish research that has a translational aspect or clinical application. Comparative physiology work that can be applied to aid the understanding human physiology is also encouraged. Manuscripts that report the use of bioinformatic, genomic, molecular, proteomic and cellular techniques to provide novel insights into integrative physiological and pathophysiological mechanisms are welcomed.
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