Effects Of Marine Lipid Fraction PCSO-524™ Supplementation On Biochemical And Functional Measures Of Muscle Damage And Soreness In Untrained Men

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2014-06
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Effects of marine lipid fraction PCSO-524™ supplementation on biochemical and functional measures of muscle damage and soreness in untrained men INTRODUCTION: Intensive or unaccustomed eccentric exercise is known to cause exercise-induced muscle damage (EIMD) commonly resulting in delayed onset muscle soreness (DOMS). EIMD/DOMS can result in decrements in endurance and resistance exercise performance. Although many treatments have been investigated for the prevention and alleviation of EIMD/DOMS, success has been limited. PCSO-524™ has been found to attenuate symptoms of inflammatory diseases such as arthritis and asthma, and thus may be a viable treatment for EIMD/DOMS and may attenuate related exercise performance decrements. PURPOSE: The purpose of this study was to examine whether or not PCSO-524™ supplementation could attenuate loss of range of motion, force loss, swelling, perceived pain through algometry and biochemical markers of inflammation, intracellular muscle proteins and oxidative stress after eccentric muscle damage. METHODS: Subjects were thirty-two healthy, untrained males aged 18–26 who had not participated in a resistance training program in the past sixty days and did not exercise for more than three times per week for 30 minutes each session. Subjects supplemented for four weeks with either PCSO-524™ (400 mg/day) or placebo, after which time participated in a 20- minute downhill run (DHR) at -16% grade. Functional measures of DOMS were measured by algometry, midline thigh girth, and maximal voluntary contraction, following supplementation and 24, 48, 72 and 96 hours following eccentric exercise. Biochemical indicators of muscle damage such as Creatine Kinase-MM, Myoglobin, Slow skeletal troponin I, Fatty Acid Binding Protein 3, Interleukin-6, Tumor Necrosis Factor Alpha, 8-hydroxy-2' -deoxyguanosine (8-OHdG), and Cardiac Troponin I was measured pre-supplementation, post-supplementation and following DHR at 0, 2, 24, 48, 72 and 96 hours. RESULTS: PCSO-524™ attenuated maximal voluntary contraction force loss significantly at 96 hours (F = 8.140 p < .001). PCSO-524™ attenuated loss of range of motion at 96 hours compared to baseline (F = 8.236 p < .05) for the PCSO-524™ group but did not change 5 for the placebo group. There was no significant change in muscle swelling from baseline as measured by thigh girth for either PCSO-524™ or placebo. There was no significant change in perceived muscle soreness as measured by algometry for either PCSO-524™ or placebo. There was significant attenuation of creatine kinase MM in the blood following EMD immediately (t = 4.467, p < .001; 95% CI = 63.0 – 169.2), 2 (t = 5.076, p < .001; 95% CI = 76.1 – 178.6), 24 (t = 12.829, p < .001; 95% CI = 562.5 – 775.6), 48 (t = 11.477, p < .001; 95% CI = 493.2 – 706.7), 72 (t =9.118, p < .001; 95% CI = 359.8 – 567.5), and 96 hours (t = 11.935, p < .001; 95% CI = 574.4 – 811.6). Significant attenuation of myoglobin occurred 24 (t = 4.334, p < .001; 95% CI = 22.9 – 63.7), 48 (t = 6.402, p < .001; 95% CI = 67.7 – 131.1), 72 (t = 5.340, p < .001; 95% CI = 119.0 – 266.3), and 96 hours (t = 3.272, p < .01; 95% CI = 49.0 – 212.3) compared to placebo. Significant attenuation of skeletal muscle troponin I occurred in the PCSO-524™ group compared to placebo 2 (t = 2.562, p < .05; 95% CI = 0.9 – 8.0), 24 (t = 3.561, p < .01; 95% CI = 4.4 – 15.4), 48 (t = 4.095, p < .001; 95% CI = 4.7 – 14.0), 72 (T = 3.222, p < .01; 95% CI = 2.5 – 11.2), and 96 hours (T = 2.177, p < .05; 95% CI = 0.3 – 10.4) post EIMD. No significant effect of supplementation status on fatty acid binding protein appearance in the blood (F = .418 p = .523) post EMID. Significant attenuation of Interleukin-6 was observed 24 (t = 3.619, p < .01; 95% CI = 3.7 – 13.3), 48 (t = 3.993, p < .001; 95% CI = 5.8 – 17.8), 72 (t = 3.621, p < .01; 95% CI = 5.0 – 17.9), and 96 hours (t = 3.076, p < .01; 95% CI = 3.1 – 15.35) post EMID compared to placebo. A significant effect of time on TNF alpha concentration in the blood (F = 132.012 p < .001) was observed 24 (t = 4.633, p < .001; 95% CI = 11.1 – 28.5), 48 (t = 4.942, p < .001; 95% CI = 10.6 – 25.7), 72 (t = 4.747, p < .001; 95% CI = 11.3 – 28.5), and 96 hours (t = 6.349, p < .001; 95% CI = 16.8 – 32.8) post EIMD. No significant effect of time on 8-OHdG concentration in the blood (F = 1.018 p .419) was observed in either the PCSO-524™ group or placebo after EIMD. No significant effect of time was observed on cTn1 concentration in the blood (F = .420 p = .889) in either PCSO-524™ or placebo after EIMD. CONCLUSIONS: Four weeks of PCSO-524™ supplementation does not improve swelling as determined by thigh girth; perceived pain by the use of algometry; appearance of Fatty Acid Binding Protein, 8-hydroxy-2' -deoxyguanosine (8-OHdG), and Cardiac Troponin I in the blood in 6 untrained males after downhill running compared to placebo. Four weeks of PCSO-524™ supplementation is effective at attenuating maximal voluntary contraction force loss; loss of range of motion; and reducing the appearance of creatine kinase-MM; skeletal muscle troponin I; interleukin-6; and Tumor Necrosis Factor- alpha in the blood in untrained males after downhill running.
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