Department of Health and Kinesiology, Exercise and Sport Nutrition Laboratory, Texas A&M University, College Station, TX 77843-4243, USA.
Department of Sports Medicine and Nutrition, Neuromuscular Research Laboratory, University of Pittsburgh, Pittsburgh, PA, 15203, Oakland.
J Int Soc Sports Nutr. 2012 Sep 13;9(1):43. doi: 10.1186/1550-2783-9-43.
Creatine monohydrate (CrM) has been consistently reported to increase muscle creatine content and improve high-intensity exercise capacity. However, a number of different forms of creatine have been purported to be more efficacious than CrM. The purpose of this study was to determine if a buffered creatine monohydrate (KA) that has been purported to promote greater creatine retention and training adaptations with fewer side effects at lower doses is more efficacious than CrM supplementation in resistance-trained individuals.
In a double-blind manner, 36 resistance-trained participants (20.2 ± 2 years, 181 ± 7 cm, 82.1 ± 12 kg, and 14.7 ± 5% body fat) were randomly assigned to supplement their diet with CrM (Creapure® AlzChem AG, Trostberg, Germany) at normal loading (4 x 5 g/d for 7-days) and maintenance (5 g/d for 21-days) doses; KA (Kre-Alkalyn®, All American Pharmaceutical, Billings, MT, USA) at manufacturer's recommended doses (KA-L, 1.5 g/d for 28-days); or, KA with equivalent loading (4 x 5 g/d for 7-days) and maintenance (5 g/d) doses of CrM (KA-H). Participants were asked to maintain their current training programs and record all workouts. Muscle biopsies from the vastus lateralis, fasting blood samples, body weight, DEXA determined body composition, and Wingate Anaerobic Capacity (WAC) tests were performed at 0, 7, and 28-days while 1RM strength tests were performed at 0 and 28-days. Data were analyzed by a repeated measures multivariate analysis of variance (MANOVA) and are presented as mean ± SD changes from baseline after 7 and 28-days, respectively.
Muscle free creatine content obtained in a subgroup of 25 participants increased in all groups over time (1.4 ± 20.7 and 11.9 ± 24.0 mmol/kg DW, p = 0.03) after 7 and 28-days, respectively, with no significant differences among groups (KA-L -7.9 ± 22.3, 4.7 ± 27.0; KA-H 1.0 ± 12.8, 9.1 ± 23.2; CrM 11.3 ± 23.9, 22.3 ± 21.0 mmol/kg DW, p = 0.46). However, while no overall group differences were observed (p = 0.14), pairwise comparison between the KA-L and CrM groups revealed that changes in muscle creatine content tended to be greater in the CrM group (KA-L -1.1 ± 4.3, CrM 11.2 ± 4.3 mmol/kg DW, p = 0.053 [mean ± SEM]). Although some significant time effects were observed, no significant group x time interactions (p > 0.05) were observed in changes in body mass, fat free mass, fat mass, percent body fat, or total body water; bench press and leg press 1RM strength; WAC mean power, peak power, or total work; serum blood lipids, markers of catabolism and bone status, and serum electrolyte status; or, whole blood makers of lymphocytes and red cells. Serum creatinine levels increased in all groups (p < 0.001) with higher doses of creatine promoting greater increases in serum creatinine (p = 0.03) but the increases observed (0.1 - 0.2 mg/dl) were well within normal values for active individuals (i.e., <1.28 ± 0.2 mg/dl). Serum LDL was decreased to a greater degree following ingesting loading doses in the CrM group but returned to baseline during the maintenance phase. No side effects were reported.
Neither manufacturers recommended doses of KA (1.5 g/d) or KA with equivalent loading (20 g/d for 7-days) and maintenance doses (5 g/d for 21-days) of CrM promoted greater changes in muscle creatine content, body composition, strength, or anaerobic capacity than CrM (20 g/d for 7-days, 5 g/d for 21-days). There was no evidence that supplementing the diet with a buffered form of creatine resulted in fewer side effects than CrM. These findings do not support claims that consuming a buffered form of creatine is a more efficacious and/or safer form of creatine to consume than creatine monohydrate.
肌酸单水合物(CrM)已被一致报道能增加肌肉肌酸含量并提高高强度运动能力。然而,许多不同形式的肌酸被认为比 CrM 更有效。本研究的目的是确定一种缓冲肌酸单水合物(KA)是否比 CrM 补充剂更有效,这种缓冲肌酸单水合物据称能在较低剂量下以较少的副作用促进更大的肌酸保留和训练适应。
在双盲的情况下,36 名经过力量训练的参与者(20.2±2 岁,181±7cm,82.1±12kg,体脂率 14.7±5%)被随机分配到以下组:正常负荷(7 天内每天 4 次,每次 5g)和维持剂量(21 天内每天 5g)补充 CrM(AlzChem AG,Trostberg,德国的 Creapure®);KA(Kre-Alkalyn®,美国的 All American Pharmaceutical,Billings,MT),按制造商建议剂量(KA-L,28 天内每天 1.5g);或,按 CrM 的相同负荷(7 天内每天 4 次,每次 5g)和维持剂量(21 天内每天 5g)补充 KA(KA-H)。参与者被要求保持他们当前的训练计划并记录所有的锻炼情况。在 0、7 和 28 天时进行股外侧肌活检、空腹血样采集、体重测量、DEXA 确定身体成分和无氧能力(Wingate Anaerobic Capacity,WAC)测试,在 0 和 28 天时进行 1RM 力量测试。数据采用重复测量多元方差分析(MANOVA)进行分析,并分别以 7 天和 28 天后的基线变化表示为均值±SD。
25 名参与者的肌肉游离肌酸含量在所有组中均随时间增加(7 天和 28 天后分别为 1.4±20.7 和 11.9±24.0mmol/kg DW,p=0.03),各组之间无显著差异(KA-L-7.9±22.3,4.7±27.0;KA-H 1.0±12.8,9.1±23.2;CrM 11.3±23.9,22.3±21.0mmol/kg DW,p=0.46)。然而,虽然没有观察到总体组间差异(p=0.14),但 KA-L 和 CrM 组之间的两两比较表明,CrM 组肌肉肌酸含量的变化趋势更大(KA-L-1.1±4.3,CrM 11.2±4.3mmol/kg DW,p=0.053[均值±SEM])。尽管观察到一些显著的时间效应,但在体重、去脂体重、体脂率、体脂百分比或总体水、卧推和腿推 1RM 力量、WAC 平均功率、峰值功率或总功、血清血脂、代谢和骨状态标志物、血清电解质状态或全血淋巴细胞和红细胞标志物的变化中没有观察到显著的组×时间相互作用(p>0.05)。血清肌酐水平在所有组中均升高(p<0.001),更高剂量的肌酸促进血清肌酐升高更大(p=0.03),但观察到的升高(0.1-0.2mg/dl)在活动个体的正常范围内(即,<1.28±0.2mg/dl)。CrM 组在负荷剂量摄入后 LDL 降低幅度更大,但在维持阶段恢复到基线。没有报告任何副作用。
按制造商建议剂量(KA-L,每天 1.5g)或与 CrM 的相同负荷(7 天内每天 4 次,每次 5g)和维持剂量(21 天内每天 5g)补充 KA 并没有比 CrM(7 天内每天 20g,21 天内每天 5g)更有效地增加肌肉肌酸含量、身体成分、力量或无氧能力。没有证据表明,与 CrM 相比,饮食中补充缓冲形式的肌酸会导致更少的副作用。这些发现不支持以下说法:即与肌酸单水合物相比,摄入缓冲形式的肌酸是一种更有效和/或更安全的肌酸形式。
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