Impacts of sarcopenia and resistance exercise training on mitochondrial quality control proteins.

IF 3.3 Q2 GERIATRICS & GERONTOLOGY

Journal of Frailty & Aging Pub Date : 2025-10-01 DOI:10.1016/j.tjfa.2025.100090

Catherine B Springer-Sapp, Olayinka O Ogbara, Odessa Addison, Sarah Kuzmiak-Glancy, Steven J Prior

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引用次数: 0

Abstract

Background: The progression of sarcopenia with aging may be related to mitochondrial dysfunction due in part to altered mitochondrial dynamics (fusion, fission, mitophagy, and biogenesis). Previous work has identified altered expression of proteins associated with these processes in with aging, but whether further changes occur in sarcopenia remains unclear.

Objectives: The purpose of this study was to assess protein expression of markers of mitochondrial fusion (Mfn2, Opa1), fission (Drp1, Fis1), mitophagy (Parkin), biogenesis (PGC-1α), and content (Complex IV: CIV) in sarcopenic and non-sarcopenic older adults. We also determined whether resistance training affected skeletal muscle mitochondrial content and expression of mitochondrial quality control proteins in sarcopenic older adults.

Design: Longitudinal exercise training study, with cross-sectional baseline comparison.

Setting and participants: Ten older adults with mild-moderate sarcopenia, plus ten non-sarcopenic, matched older adults from Maryland, USA.

Intervention: Twelve-week resistance training.

Measurements: Strength, sarcopenic index (ALM/BMI: appendicular lean mass divided by body mass index), body composition, and mitochondrial morphology and protein expression in vastus lateralis muscle.

Results: No differences in protein expression were observed between sarcopenic and non-sarcopenic participants at baseline; however, ALM/BMI was inversely related to CIV expression (r = -0.55, P = 0.013) across all subjects. Similarly, lean body mass and ALM correlated inversely with expression of the fusion protein Opa1-S (r = -0.55 - -0.51, P ≤ 0.022). Resistance training increased strength in sarcopenic older adults by 13 % (P = 0.02), but this group's expression of mitochondrial quality control proteins was mostly unaltered.

Conclusions: The presence of sarcopenia identified by ALM/BMI was not associated with changes in protein expression that are consistent with impaired mitochondrial dynamics beyond those changes that might occur with aging alone. While short-term resistance training increased strength in older adults with sarcopenia, this was not accompanied by changes in protein expression, with the possible exception of fusion protein Mfn2.

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肌肉减少症和阻力运动训练对线粒体质量控制蛋白的影响。

背景：随着年龄的增长，肌肉减少症的进展可能与线粒体功能障碍有关，部分原因是线粒体动力学（融合、裂变、线粒体自噬和生物发生）的改变。先前的研究已经确定了与衰老过程相关的蛋白质表达的改变，但是否在肌肉减少症中发生进一步的变化仍不清楚。目的：本研究的目的是评估肌少症和非肌少症老年人线粒体融合（Mfn2, Opa1），裂变（Drp1, Fis1），线粒体自噬（Parkin），生物发生（PGC-1α）和含量（复合体IV: CIV）标志物的蛋白表达。我们还确定了阻力训练是否影响骨骼肌线粒体含量和线粒体质量控制蛋白的表达。设计：纵向运动训练研究，横断面基线比较。环境和参与者：10名患有轻中度肌肉减少症的老年人加上10名非肌肉减少症的老年人，来自美国马里兰州。干预：12周的抗阻训练。测量：力量、肌肉减少指数（ALM/BMI：阑尾瘦体重除以体重指数）、体成分、股外侧肌线粒体形态和蛋白质表达。结果：基线时肌少症患者和非肌少症患者的蛋白表达无差异；然而，所有受试者的ALM/BMI与CIV表达呈负相关（r = -0.55, P = 0.013）。同样，瘦体重和ALM与融合蛋白Opa1-S的表达呈负相关（r = -0.55 ~ -0.51, P≤0.022）。阻力训练使肌肉减少的老年人的力量增加了13% (P = 0.02)，但这一组的线粒体质量控制蛋白的表达基本没有改变。结论：ALM/BMI鉴定的肌少症的存在与蛋白质表达的变化无关，蛋白质表达的变化与线粒体动力学受损一致，而这些变化可能仅与衰老有关。虽然短期阻力训练增加了老年肌肉减少症患者的力量，但这并不伴随着蛋白表达的变化，可能融合蛋白Mfn2除外。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Frailty & Aging GERIATRICS & GERONTOLOGY-

CiteScore

5.90

自引率

7.70%

发文量

期刊介绍： The Journal of Frailty & Aging is a peer-reviewed international journal aimed at presenting articles that are related to research in the area of aging and age-related (sub)clinical conditions. In particular, the journal publishes high-quality papers describing and discussing social, biological, and clinical features underlying the onset and development of frailty in older persons. The Journal of Frailty & Aging is composed by five different sections: - Biology of frailty and aging In this section, the journal presents reports from preclinical studies and experiences focused at identifying, describing, and understanding the subclinical pathophysiological mechanisms at the basis of frailty and aging. - Physical frailty and age-related body composition modifications Studies exploring the physical and functional components of frailty are contained in this section. Moreover, since body composition plays a major role in determining physical frailty and, at the same time, represents the most evident feature of the aging process, special attention is given to studies focused on sarcopenia and obesity at older age. - Neurosciences of frailty and aging The section presents results from studies exploring the cognitive and neurological aspects of frailty and age-related conditions. In particular, papers on neurodegenerative conditions of advanced age are welcomed. - Frailty and aging in clinical practice and public health This journal’s section is devoted at presenting studies on clinical issues of frailty and age-related conditions. This multidisciplinary section particularly welcomes reports from clinicians coming from different backgrounds and specialties dealing with the heterogeneous clinical manifestations of advanced age. Moreover, this part of the journal also contains reports on frailty- and age-related social and public health issues. - Clinical trials and therapeutics This final section contains all the manuscripts presenting data on (pharmacological and non-pharmacological) interventions aimed at preventing, delaying, or treating frailty and age-related conditions.The Journal of Frailty & Aging is a quarterly publication of original papers, review articles, case reports, controversies, letters to the Editor, and book reviews. Manuscripts will be evaluated by the editorial staff and, if suitable, by expert reviewers assigned by the editors. The journal particularly welcomes papers by researchers from different backgrounds and specialities who may want to share their views and experiences on the common themes of frailty and aging.The abstracting and indexing of the Journal of Frailty & Aging is covered by MEDLINE (approval by the National Library of Medicine in February 2016).