p38α kinase governs muscle strength through PGC1α in mice

IF 5.6 2区 医学 Q1 PHYSIOLOGY Acta Physiologica Pub Date : 2024-10-03 DOI:10.1111/apha.14234
Leticia Herrera-Melle, Beatriz Cicuéndez, Juan Antonio López, Phillip A. Dumesic, Sarah E. Wilensky, Elena Rodríguez, Luis Leiva-Vega, Ainoa Caballero, Marta León, Jesús Vázquez, Bruce M. Spiegelman, Cintia Folgueira, Alfonso Mora, Guadalupe Sabio
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Abstract

Aims

Skeletal muscle, with its remarkable plasticity and dynamic adaptation, serves as a cornerstone of locomotion and metabolic homeostasis in the human body. Muscle tissue, with its extraordinary capacity for force generation and energy expenditure, plays a fundamental role in the movement, metabolism, and overall health. In this context, we sought to determine the role of p38α in mitochondrial metabolism since mitochondrial dynamics play a crucial role in the development of muscle-related diseases that result in muscle weakness.

Methods

We conducted our study using male mice (MCK-cre, p38αMCK-KO and PGC1α MCK-KO) and mouse primary myoblasts. We analyzed mitochondrial metabolic, physiological parameters as well as proteomics, western blot, RNA-seq analysis from muscle samples.

Results

Our findings highlight the critical involvement of muscle p38α in the regulation of mitochondrial function, a key determinant of muscle strength. The absence of p38α triggers changes in mitochondrial dynamics through the activation of PGC1α, a central regulator of mitochondrial biogenesis. These results have substantial implications for understanding the complex interplay between p38α kinase, PGC1α activation, and mitochondrial content, thereby enhancing our knowledge in the control of muscle biology.

Conclusions

This knowledge holds relevance for conditions associated with muscle weakness, where disruptions in these molecular pathways are frequently implicated in diminishing physical strength. Our research underscores the potential importance of targeting the p38α and PGC1α pathways within muscle, offering promising avenues for the advancement of innovative treatments. Such interventions hold the potential to improve the quality of life for individuals affected by muscle-related diseases.

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p38α 激酶通过 PGC1α 调节小鼠肌肉力量
目的:骨骼肌具有显著的可塑性和动态适应性,是人体运动和新陈代谢平衡的基石。肌肉组织具有非凡的发力和能量消耗能力,在运动、新陈代谢和整体健康中发挥着重要作用。在这种情况下,我们试图确定 p38α 在线粒体代谢中的作用,因为线粒体动力学在导致肌无力的肌肉相关疾病的发展中起着至关重要的作用:我们使用雄性小鼠(MCK-cre、p38αMCK-KO 和 PGC1α MCK-KO)和小鼠原代成肌细胞进行了研究。我们对肌肉样本的线粒体代谢、生理参数以及蛋白质组学、Western blot、RNA-seq分析进行了分析:结果:我们的研究结果突显了肌肉 p38α 在线粒体功能调控中的关键作用,而线粒体功能是决定肌肉力量的关键因素。p38α 的缺失会通过激活线粒体生物生成的核心调节因子 PGC1α 引发线粒体动力学的变化。这些结果对理解 p38α 激酶、PGC1α 激活和线粒体含量之间复杂的相互作用具有重要意义,从而增强了我们在肌肉生物学控制方面的知识:这些知识对与肌肉无力相关的疾病具有现实意义,因为这些分子通路的破坏往往与体力下降有关。我们的研究强调了以肌肉中的 p38α 和 PGC1α 通路为靶点的潜在重要性,为推进创新治疗提供了前景广阔的途径。这些干预措施有望改善肌肉相关疾病患者的生活质量。
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来源期刊
Acta Physiologica
Acta Physiologica 医学-生理学
CiteScore
11.80
自引率
15.90%
发文量
182
审稿时长
4-8 weeks
期刊介绍: Acta Physiologica is an important forum for the publication of high quality original research in physiology and related areas by authors from all over the world. Acta Physiologica is a leading journal in human/translational physiology while promoting all aspects of the science of physiology. The journal publishes full length original articles on important new observations as well as reviews and commentaries.
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