首页> 外文期刊>Journal of the International Society of Sports Nutrition >Can a standard dose of eicosapentaenoic acid (EPA) supplementation reduce the symptoms of delayed onset of muscle soreness?
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Can a standard dose of eicosapentaenoic acid (EPA) supplementation reduce the symptoms of delayed onset of muscle soreness?

机译:标准剂量的二十碳五烯酸(EPA)补充剂可以减轻肌肉酸痛延迟发作的症状吗?

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Background Unaccustomed exercise can result in delayed onset of muscle soreness (DOMS) which can affect athletic performance. Although DOMS is a useful tool to identify muscle damage and remodelling, prolonged symptoms of DOMS may be associated with the over-training syndrome. In order to reduce the symptoms of DOMS numerous management strategies have been attempted with no significant effect on DOMS-associated cytokines surge. The present study aimed to investigate the acute and chronic effects of a 2 × 180 mg per day dose of eicosapentaenoic acid (EPA) on interleukin-6 (IL-6) mediated inflammatory response and symptoms associated with DOMS. Methods Seventeen healthy non-smoking females (age 20.4 ± 2.1 years, height 161.2 ± 8.3 cm and mass 61.48 ± 7.4 kg) were randomly assigned to either placebo (N = 10) or EPA (N = 7). Serum IL-6, isometric and isokinetic (concentric and eccentric) strength, and rating of perceived exertion (RPE) were recorded on four occasions: i-prior to supplementation, ii-immediately after three weeks of supplementation (basal effects), iii-48 hours following a single bout of resistance exercise (acute training response effects), and iv-48 hours following the last of a series of three bouts of resistance exercise (chronic training response effects). Results There was only a group difference in the degree of change in circulating IL-6 levels. In fact, relative to the first baseline, by the third bout of eccentric workout, the EPA group had 103 ± 60% increment in IL-6 levels whereas the placebo group only had 80 ± 26% incremented IL-6 levels (P = 0.020). We also describe a stable multiple linear regression model which included measures of strength and not IL-6 as predictors of RPE scale. Conclusion The present study suggests that in doubling the standard recommended dose of EPA, whilst this may still not be beneficial at ameliorating the symptoms of DOMS, it counter intuitively appears to enhance the cytokine response to exercise. In a context where previous in vitro work has shown EPA to decrease the effects of inflammatory cytokines, it may in fact be that the doses required in vivo is much larger than current recommended amounts. An attempt to dampen the exercise-induced cytokine flux in fact results in an over-compensatory response of this system.
机译:背景技术不习惯的运动可能会导致肌肉酸痛(DOMS)发作延迟,从而影响运动表现。尽管DOMS是识别肌肉损伤和重塑的有用工具,但DOMS症状延长可能与过度训练综合症有关。为了减轻DOMS的症状,已经尝试了多种治疗策略,这些策略对DOMS相关的细胞因子激增没有明显的影响。本研究旨在调查每天2×180 mg二十碳五烯酸(EPA)对白介素6(IL-6)介导的炎症反应和与DOMS相关的症状的急性和慢性作用。方法将17名健康的非吸烟女性(年龄20.4±2.1岁,身高161.2±8.3厘米,体重61.48±7.4千克)随机分配至安慰剂组(N = 10)或EPA(N = 7)。在以下四种情况下记录了血清IL-6,等距和等速(同心和偏心)强度以及感知的劳累力(RPE)等级:补充前i,补充三周后立即(基础效果),iii-一次单次抵抗运动后48小时(急性训练反应效果),以​​及一系列三次抵抗运动后最后一次IV-48小时(慢性训练反应效果)。结果循环IL-6水平的变化程度仅有一组差异。实际上,相对于第一个基线,到第三次偏心锻炼,EPA组的IL-6水平增加了103±60%,而安慰剂组的IL-6水平仅增加了80±26%(P = 0.020 )。我们还描述了一个稳定的多元线性回归模型,该模型包括强度指标,而非IL-6作为RPE量表的预测指标。结论本研究表明,将EPA的标准推荐剂量加倍,尽管这可能仍不足以改善DOMS的症状,但从直觉上看,它似乎增强了细胞因子对运动的反应。在先前的体外研究表明EPA可以降低炎症细胞因子的作用的情况下,实际上可能是体内所需的剂量比目前的建议剂量大得多。试图抑制运动引起的细胞因子通量实际上导致该系统的过度补偿反应。

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