Center for Cardiometabolic Science, Christina Lee Brown Envirome Institute, Division of Environmental Medicine, Department of Medicine, University of Louisville, Louisville, KY, United States of America.
Center for Environmental and Systems Biochemistry, University of Kentucky, Lexington, KY, United States of America.
J Mol Cell Cardiol. 2024 Jun;191:50-62. doi: 10.1016/j.yjmcc.2024.04.014. Epub 2024 May 3.
Exercise training can promote physiological cardiac growth, which has been suggested to involve changes in glucose metabolism to facilitate hypertrophy of cardiomyocytes. In this study, we used a dietary, in vivo isotope labeling approach to examine how exercise training influences the metabolic fate of carbon derived from dietary glucose in the heart during acute, active, and established phases of exercise-induced cardiac growth. Male and female FVB/NJ mice were subjected to treadmill running for up to 4 weeks and cardiac growth was assessed by gravimetry. Cardiac metabolic responses to exercise were assessed via in vivo tracing of [C]-glucose via mass spectrometry and nuclear magnetic resonance. We found that the half-maximal cardiac growth response was achieved by approximately 1 week of daily exercise training, with near maximal growth observed in male mice with 2 weeks of training; however, female mice were recalcitrant to exercise-induced cardiac growth and required a higher daily intensity of exercise training to achieve significant, albeit modest, increases in cardiac mass. We also found that increases in the energy charge of adenylate and guanylate nucleotide pools precede exercise-induced changes in cardiac size and were associated with higher glucose tracer enrichment in the TCA pool and in amino acids (aspartate, glutamate) sourced by TCA intermediates. Our data also indicate that the activity of collateral biosynthetic pathways of glucose metabolism may not be markedly altered by exercise. Overall, this study provides evidence that metabolic remodeling in the form of heightened energy charge and increased TCA cycle activity and cataplerosis precedes cardiac growth caused by exercise training in male mice.
运动训练可以促进心脏的生理生长,这被认为涉及葡萄糖代谢的变化,以促进心肌细胞的肥大。在这项研究中,我们使用了一种饮食、体内同位素标记方法,来研究运动训练在急性、活跃和已建立的运动诱导心脏生长阶段,如何影响来自饮食葡萄糖的碳在心脏中的代谢命运。雄性和雌性 FVB/NJ 小鼠接受跑步机跑步训练长达 4 周,并通过称重评估心脏生长。通过质谱和核磁共振对[C]-葡萄糖的体内追踪,评估心脏对运动的代谢反应。我们发现,大约 1 周的日常运动训练就可以达到心脏生长的半最大反应,2 周的训练可以使雄性小鼠的心脏生长接近最大;然而,雌性小鼠对运动诱导的心脏生长具有抵抗力,需要更高的日常运动训练强度才能使心脏质量显著增加,但增加幅度较小。我们还发现,腺苷酸和鸟苷酸核苷酸池的能量电荷增加先于心脏大小的运动诱导变化,并且与 TCA 池和 TCA 中间体来源的氨基酸(天冬氨酸、谷氨酸)中的葡萄糖示踪剂富集有关。我们的数据还表明,葡萄糖代谢的旁生生物合成途径的活性可能不会因运动而明显改变。总的来说,这项研究提供了证据表明,在雄性小鼠中,运动训练引起的心脏生长之前,存在以高能电荷和增加的 TCA 循环活性和脱羧作用为形式的代谢重塑。