炎症在线粒体功能障碍和肌肉疏松症之间的中介作用:综述。

IF 1.4 Q4 IMMUNOLOGY
American journal of clinical and experimental immunology Pub Date : 2023-12-15 eCollection Date: 2023-01-01
Xin Xu, Zixing Wen
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引用次数: 0

摘要

骨质疏松症的特点是骨骼肌质量和力量的隐性减少,对老年人群的生活质量造成了不利影响。目前的治疗策略仅限于物理治疗干预,这表明迫切需要阐明病因基础,以促进创新药物疗法的开发。最近的科学研究发现,线粒体功能障碍和炎症与肌肉疏松症的病因有关。线粒体是肌肉组织内许多基本细胞过程的组成部分,包括但不限于细胞凋亡、自噬、通过活性氧发出信号以及维持蛋白质平衡。线粒体动力学的偏差,再加上氧化能力、自噬过程和蛋白质平衡受到损害,会导致肌肉结构和功能紊乱。线粒体功能障碍尤其有害,因为它会降低氧化磷酸化,加剧细胞凋亡活动,并阻碍肌肉细胞内的钙平衡。此外,呼吸恶化、氧化损伤加剧和质量控制机制减弱等有害的反馈回路会加速肌肉衰老。值得注意的是,线粒体表现出的能量代谢缺陷是促使肌肉从正常衰老状态转变为致病状态的关键因素。这篇分析性综述细致研究了线粒体功能障碍、持续炎症和肌肉疏松症发病机制之间复杂的相互作用。它强调了在老年群体中缓解炎症和修正线粒体异常作为预防和控制肌肉疏松症策略的必要性。文章首先概述了肌肉疏松症及其临床影响。接着,文章探讨了线粒体功能障碍与肌肉疏松症发生之间的直接关系。同时,它还强调了骨骼肌衰老过程中炎症反应和线粒体功能不足之间潜在的协同效应,从而阐明了新出现的治疗目标。最后,这篇综述提炼了目前对与肌肉疏松症有关的线粒体和炎症途径的理解,并勾勒出现存的知识空白,为后续的科学探索指明了方向。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The mediating role of inflammaging between mitochondrial dysfunction and sarcopenia in aging: a review.

Sarcopenia, characterized by the insidious reduction of skeletal muscle mass and strength, detrimentally affects the quality of life in elderly cohorts. Present therapeutic strategies are confined to physiotherapeutic interventions, signaling a critical need for elucidation of the etiological underpinnings to facilitate the development of innovative pharmacotherapies. Recent scientific inquiries have associated mitochondrial dysfunction and inflammation with the etiology of sarcopenia. Mitochondria are integral to numerous fundamental cellular processes within muscle tissue, including but not limited to apoptosis, autophagy, signaling via reactive oxygen species, and the maintenance of protein equilibrium. Deviations in mitochondrial dynamics, coupled with compromised oxidative capabilities, autophagic processes, and protein equilibrium, result in disturbances to muscular architecture and functionality. Mitochondrial dysfunction is particularly detrimental as it diminishes oxidative phosphorylation, escalates apoptotic activity, and hinders calcium homeostasis within muscle cells. Additionally, deleterious feedback loops of deteriorated respiration, exacerbated oxidative injury, and diminished quality control mechanisms precipitate the acceleration of muscular senescence. Notably, mitochondria exhibiting deficient energetic metabolism are pivotal in precipitating the shift from normative muscle aging to a pathogenic state. This analytical review meticulously examines the complex interplay between mitochondrial dysfunction, persistent inflammation, and the pathogenesis of sarcopenia. It underscores the imperative to alleviate inflammation and amend mitochondrial anomalies within geriatric populations as a strategy to forestall and manage sarcopenia. An initial overview provides a succinct exposition of sarcopenia and its clinical repercussions. The discourse then progresses to an examination of the direct correlation between mitochondrial dysfunction and the genesis of sarcopenia. Concomitantly, it accentuates potential synergistic effects between inflammatory responses and mitochondrial insufficiencies during the aging of skeletal muscle, thereby casting light upon emergent therapeutic objectives. In culmination, this review distills the prevailing comprehension of the mitochondrial and inflammatory pathways implicated in sarcopenia and delineates extant lacunae in knowledge to orient subsequent scientific inquiry.

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