在人体骨骼肌中,SIRT3基因表达会因禁食和运动而改变,但SIRT3的亚细胞定位不变。
SIRT3 gene expression but not SIRT3 subcellular localization is altered in response to fasting and exercise in human skeletal muscle.
作者信息
Edgett Brittany A, Hughes Meghan C, Matusiak Jennifer B L, Perry Christopher G R, Simpson Craig A, Gurd Brendon J
机构信息
School of Kinesiology and Health Studies, Queen's University, Kingston, Ontario, Canada, K7L 3N6.
School of Kinesiology and Health Science, Muscle Health Research Centre, York University, Toronto, Ontario, Canada, M3J 1P3.
出版信息
Exp Physiol. 2016 Aug 1;101(8):1101-13. doi: 10.1113/EP085744.
What is the central question of this study? Evidence from cellular and animal models suggests that SIRT3 is involved in regulating aerobic ATP production. Thus, we investigated whether changes in fatty acid and oxidative metabolism known to accompany fasting and exercise occur in association with changes in SIRT3 mitochondrial localization and expression in human skeletal muscle. What is the main finding and its importance? We find that 48 h of fasting and acute endurance exercise decrease SIRT3 mRNA expression but do not alter SIRT3 mitochondrial localization despite marked increases in fatty acid oxidation. This suggests that SIRT3 activity is not regulated by changes in mitochondrial localization in response to cellular energy stress in human skeletal muscle. The present study examined SIRT3 expression and SIRT3 mitochondrial localization in response to acute exercise and short-term fasting in human skeletal muscle. Experiment 1 involved eight healthy men (age, 21.4 ± 2.8 years; peak O2 uptake, 47.1 ± 11.8 ml min(-1) kg(-1) ) who performed a single bout of exercise at ∼55% of peak aerobic work rate for 1 h. Muscle biopsies were obtained at rest (Rest), immediately after exercise (EX-0) and 3 h postexercise (EX-3). Experiment 2 involved 10 healthy men (age, 22.0 ± 1.5 years; peak O2 uptake, 46.9 ± 6.0 ml min−1 kg−1) who underwent a 48 h fast, with muscle biopsies collected 1 h postprandial (Fed) and after 48 h of fasting (Fast). Mitochondrial respiration was measured using high-resolution respirometry in permeabilized muscle fibre bundles to assess substrate oxidation. Whole body fat oxidation increased after both exercise (Rest, 0.96 ± 0.32 kcal min(-1) ; Exercise, 5.66 ± 1.97 kcal min(-1) ; P < 0.001) and fasting (Fed, 0.87 ± 0.51 kcal min(-1) ; Fast, 1.30 ± 0.37 kcal min(-1) , P < 0.05). SIRT3 gene expression decreased (P < 0.05) after both exercise (-8%) and fasting (-19%); however, SIRT3 whole muscle protein content was unaltered after fasting. No changes were observed in SIRT3 mitochondrial localization following either exercise or fasting. Fasting also decreased the Vmax of glutamate [80 ± 43 versus 50 ± 21 pmol s(-1) (mg dry weight)(-1) ; P < 0.05]. These findings suggest that SIRT3 does not appear to be regulated by changes in mitochondrial localization at the time points measured in the present study in response to cellular energy stress in human skeletal muscle.
本研究的核心问题是什么?细胞和动物模型的证据表明,SIRT3参与调节有氧ATP的产生。因此,我们研究了已知与禁食和运动相关的脂肪酸和氧化代谢变化是否与人类骨骼肌中SIRT3的线粒体定位及表达变化有关。主要发现及其重要性是什么?我们发现,尽管脂肪酸氧化显著增加,但48小时禁食和急性耐力运动可降低SIRT3 mRNA表达,但不改变SIRT3的线粒体定位。这表明,在人类骨骼肌中,SIRT3的活性不受细胞能量应激导致的线粒体定位变化的调节。本研究检测了人类骨骼肌在急性运动和短期禁食后的SIRT3表达及SIRT3的线粒体定位。实验1中,8名健康男性(年龄21.4±2.8岁;峰值摄氧量47.1±11.8 ml·min⁻¹·kg⁻¹)以约55%的峰值有氧工作率进行了1小时的单次运动。在静息状态(Rest)、运动后即刻(EX - 0)和运动后3小时(EX - 3)采集肌肉活检样本。实验2中,10名健康男性(年龄22.0±1.5岁;峰值摄氧量46.9±6.0 ml·min⁻¹·kg⁻¹)进行了48小时禁食,在餐后1小时(Fed)和禁食48小时后(Fast)采集肌肉活检样本。使用高分辨率呼吸测定法测量透化肌纤维束中的线粒体呼吸,以评估底物氧化。运动(静息状态下,0.96±0.32 kcal·min⁻¹;运动后,5.66±1.97 kcal·min⁻¹;P<0.001)和禁食(餐后,0.87±0.51 kcal·min⁻¹;禁食后,1.30±0.37 kcal·min⁻¹,P<0.05)后,全身脂肪氧化均增加。运动(-8%)和禁食(-19%)后,SIRT3基因表达均下降(P<0.05);然而,禁食后SIRT3全肌肉蛋白含量未改变。运动或禁食后,SIRT3的线粒体定位均未观察到变化。禁食还降低了谷氨酸的最大反应速度[80±43对50±21 pmol·s⁻¹·(mg干重)⁻¹;P<0.05]。这些发现表明,在本研究测量的时间点上,人类骨骼肌中SIRT3似乎不受细胞能量应激导致的线粒体定位变化的调节。
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