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首页> 外文期刊>American Journal of Physiology >A systems-based investigation into vitamin D and skeletal muscle repair, regeneration, and hypertrophy
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A systems-based investigation into vitamin D and skeletal muscle repair, regeneration, and hypertrophy

机译:基于系统的维生素D和骨骼肌修复,再生和肥大的调查

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Skeletal muscle is a direct target for vitamin D. Observational studies suggest that low 25[OH]D correlates with functional recovery of skeletal muscle following eccentric contractions in humans and crush injury in rats. However, a definitive association is yet to be established. To address this gap in knowledge in relation to damage repair, a randomised, placebo-controlled trial was performed in 20 males with insufficient concentrations of serum 25(OH)D (45 ± 25 nmol/l). Prior to and following 6 wk of supplemental vitamin D_3 (4,000 Ш/day) or placebo (50 mg of cellulose), participants performed 20 × 10 damaging eccentric contractions of the knee extensors, with peak torque measured over the following 7 days of recovery. Parallel experimentation using isolated human skeletal muscle-derived myo-blast cells from biopsies of 14 males with low serum 25(OH)D (37 ± 11 nmol/l) were subjected to mechanical wound injury, which enabled corresponding in vitro studies of muscle repair, regeneration, and hypertrophy in the presence and absence of 10 or 100 nmol 1alpha,25(OH)_2D_3. Supplemental vitamin D_3 increased serum 25(OH)D and improved recovery of peak torque at 48 h and 7 days postexercise. In vitro, 10 nmol 1alpha,25(OH)_2D_3 improved muscle cell migration dynamics and resulted in improved myotube fusion/differentiation at the biochemical, morphological, and molecular level together with increased myotube hypertrophy at 7 and 10 days postdamage. Together, these preliminary data are the first to characterize a role for vitamin D in human skeletal muscle regeneration and suggest that maintaining serum 25(OH)D may be beneficial for enhancing repar-ative processes and potentially for facilitating subsequent hypertrophy.
机译:骨骼肌是维生素D的直接靶标。观察研究表明,低25 [OH] D与人类偏心收缩后骨骼肌功能恢复相关,大鼠挤压损伤。但是,尚未建立过定的关联。为了解决与损伤修复有关的知识中的这种差距,在20个雄性中进行随机的安慰剂对照试验,浓度不足的血清25(OH)D(45±25 Nmol / L)。在此之前和以下6周期的补充维生素D_3(4,000×/日)或安慰剂(50mg纤维素)之前,参与者进行了20×10损伤膝盖伸肌的偏心收缩,并且在恢复后7天测量峰值扭矩。使用从14个血清中的14个男性的活组织检查中使用分离的人骨骼肌衍生的肌肌肌肌肌肌肌肌肌肌肌肌肌肌肌肌肌肌肌肌肌肿块进行机械伤口损伤,这使能相应的肌肉修复体外研究在存在和不存在10或100nmol 1Alpha,25(OH)_2d_3的情况下,再生和肥大。补充维生素D_3增加了血清25(OH)D,并在第二秒钟内提高了峰值扭矩的回收率和7天。体外,10nmol 1Alpha,25(OH)_2D_3改善了肌肉细胞迁移动态,并导致生化,形态学和分子水平的肌肌管融合/分化,并在7和10天在初期增加myotube肥大。这些初步数据在一起是首先表征维生素D在人骨骼肌再生中的作用,并表明维持血清25(OH)D可以有利于提高归因于恢复过程,并且可能促进随后的肥大。

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