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缺血预适应的促效作用并非通过血液直接传递到分离的骨骼肌。

Ergogenic effect of ischemic preconditioning is not directly conferred to isolated skeletal muscle via blood.

机构信息

Human Performance & Health Research Laboratory, Department of Human Health and Nutritional Sciences, University of Guelph, Guelph, ON, Canada.

Department of Human Health and Nutritional Sciences, University of Guelph, Guelph, ON, Canada.

出版信息

Eur J Appl Physiol. 2023 Aug;123(8):1851-1861. doi: 10.1007/s00421-023-05197-1. Epub 2023 Apr 19.

Abstract

PURPOSE

Ischemic preconditioning (IPC) in humans has been demonstrated to confer ergogenic benefit to aerobic exercise performance, with an improvement in the response rate when the IPC stimulus is combined with concurrent exercise. Despite potential performance improvements, the nature of the neuronal and humoral mechanisms of conferral and their respective contributions to ergogenic benefit remain unclear. We sought to examine the effects of the humoral component of ischemic preconditioning on skeletal muscle tissue using preconditioned human serum and isolated mouse soleus.

METHODS

Isolated mouse soleus was electrically stimulated to contract while in human serum preconditioned with either traditional (IPC) or augmented (AUG) ischemic preconditioning compared to control (CON) and exercise (ERG) preconditioning. Force frequency (FF) curves, twitch responses, and a fatigue-recovery protocol were performed on muscles before and after the addition of serum. After preconditioning, human participants performed a 4 km cycling time trial in order to identify responders and non-responders to IPC.

RESULTS

No differences in indices of contractile function, fatiguability, nor recovery were observed between conditions in mouse soleus muscles. Further, no human participants improved performance in a 4-km cycling time trial in response to traditional nor augmented ischemic preconditioning compared to control or exercise conditions (CON 407.7 ± 41.1 s, IPC 411.6 ± 41.9 s, ERG 408.8 ± 41.4 s, AUG 414.1 ± 41.9 s).

CONCLUSIONS

Our findings do not support the conferral of ergogenic benefit via a humoral component of IPC at the intracellular level. Ischemic preconditioning may not manifest prominently at submaximal exercise intensities, and augmented ischemic preconditioning may have a hormetic relationship with performance improvements.

摘要

目的

在人体中已经证明,缺血预处理(IPC)可以为有氧运动表现带来增益作用,当 IPC 刺激与同时进行的运动相结合时,反应率会提高。尽管可能会提高运动表现,但赋予增益作用的神经元和体液机制的性质及其各自对增益作用的贡献仍不清楚。我们试图使用预处理的人血清和分离的小鼠比目鱼肌来研究缺血预处理的体液成分对骨骼肌组织的影响。

方法

在人血清中进行传统(IPC)或增强(AUG)缺血预处理,与对照(CON)和运动(ERG)预处理相比,对分离的小鼠比目鱼肌进行电刺激收缩。在添加血清前后,对肌肉进行力频(FF)曲线、抽搐反应和疲劳恢复协议的测试。在预处理后,人类参与者进行了 4 公里的自行车计时赛,以确定对 IPC 的反应者和非反应者。

结果

在小鼠比目鱼肌中,收缩功能、疲劳性和恢复能力的指标在不同条件之间没有差异。此外,与对照或运动条件相比,传统或增强的缺血预处理并未使人类参与者在 4 公里自行车计时赛中提高表现(CON 407.7±41.1 s,IPC 411.6±41.9 s,ERG 408.8±41.4 s,AUG 414.1±41.9 s)。

结论

我们的发现不支持 IPC 的体液成分在细胞内水平赋予增益作用。缺血预处理可能不会在亚最大运动强度下明显表现出来,而增强的缺血预处理可能与表现的改善存在一种兴奋效应关系。

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