Department of Kinesiology and Physical Education, McGill University, Montreal, Quebec, Canada.
Research Institute of the McGill University Health Centre, Montreal, Quebec, Canada.
Am J Physiol Cell Physiol. 2024 Jun 1;326(6):C1769-C1775. doi: 10.1152/ajpcell.00207.2024. Epub 2024 Apr 29.
We recently demonstrated that acute oral ketone monoester intake induces a stimulation of postprandial myofibrillar protein synthesis rates comparable to that elicited following the ingestion of 10 g whey protein or their coingestion. The present investigation aimed to determine the acute effects of ingesting a ketone monoester, whey protein, or their coingestion on mechanistic target of rapamycin (mTOR)-related protein-protein colocalization and intracellular trafficking in human skeletal muscle. In a randomized, double-blind, parallel group design, 36 healthy recreationally active young males (age: 24.2 ± 4.1 yr) ingested either: ) 0.36 g·kg bodyweight of the ketone monoester (R)-3-hydroxybutyl (R)-3-hydroxybutyrate (KET), ) 10 g whey protein (PRO), or ) the combination of both (KET + PRO). Muscle biopsies were obtained in the overnight postabsorptive state (basal conditions), and at 120 and 300 min in the postprandial period for immunofluorescence assessment of protein translocation and colocalization of mTOR-related signaling molecules. All treatments resulted in a significant (Interaction: < 0.0001) decrease in tuberous sclerosis complex 2 (TSC2)-Ras homolog enriched in brain (Rheb) colocalization at 120 min versus basal; however, the decrease was sustained at 300 min versus basal ( < 0.0001) only in KET + PRO. PRO and KET + PRO increased (Interaction: < 0.0001) mTOR-Rheb colocalization at 120 min versus basal; however, KET + PRO resulted in a sustained increase in mTOR-Rheb colocalization at 300 min that was greater than KET and PRO. Treatment intake increased mTOR-wheat germ agglutinin (WGA) colocalization at 120 and 300 min (Time: = 0.0031), suggesting translocation toward the fiber periphery. These findings demonstrate that ketone monoester intake can influence the spatial mechanisms involved in the regulation of mTORC1 in human skeletal muscle. We explored the effects of a ketone monoester (KET), whey protein (PRO), or their coingestion (KET + PRO) on mTOR-related protein-protein colocalization and intracellular trafficking in human muscle. All treatments decreased TSC2-Rheb colocalization at 120 minutes; however, KET + PRO sustained the decrease at 300 min. Only PRO and KET + PRO increased mTOR-Rheb colocalization; however, the increase at 300 min was greater in KET + PRO. Treatment intake increased mTOR-WGA colocalization, suggesting translocation to the fiber periphery. Ketone bodies influence the spatial regulation of mTOR.
我们最近证明,急性口服酮单酯摄入可刺激餐后肌纤维蛋白合成率的增加,其效果可与摄入 10 克乳清蛋白或两者同时摄入相当。本研究旨在确定摄入酮单酯、乳清蛋白或两者同时摄入对人体骨骼肌中雷帕霉素靶蛋白(mTOR)相关蛋白-蛋白共定位和细胞内运输的急性影响。在一项随机、双盲、平行组设计中,36 名健康的业余年轻男性(年龄:24.2±4.1 岁)摄入以下三种处理之一:)0.36 克/公斤体重的酮单酯(R)-3-羟基丁酸(R)-3-羟基丁酸酯(KET),)10 克乳清蛋白(PRO),或)两者的组合(KET+PRO)。在隔夜禁食后吸收状态(基础条件)以及餐后 120 和 300 分钟时,通过免疫荧光评估蛋白质转位和 mTOR 相关信号分子的共定位,获取肌肉活检。所有处理均导致雷帕霉素复合物 2(TSC2)-富含大脑的 Ras 同源物(Rheb)共定位在 120 分钟时与基础相比显著降低(交互作用:<0.0001);然而,与基础相比,仅在 KET+PRO 时,这种降低在 300 分钟时持续存在(<0.0001)。PRO 和 KET+PRO 在 120 分钟时增加 mTOR-Rheb 共定位(交互作用:<0.0001);然而,KET+PRO 导致 mTOR-Rheb 共定位在 300 分钟时持续增加,高于 KET 和 PRO。处理摄入增加了 mTOR-小麦胚凝集素(WGA)在 120 和 300 分钟时的共定位(时间:=0.0031),提示向纤维外周转运。这些发现表明,酮单酯摄入可以影响人类骨骼肌中 mTORC1 调节的空间机制。我们探讨了酮单酯(KET)、乳清蛋白(PRO)或两者同时摄入(KET+PRO)对人肌肉中 mTOR 相关蛋白-蛋白共定位和细胞内运输的影响。所有处理均在 120 分钟时降低 TSC2-Rheb 共定位;然而,KET+PRO 在 300 分钟时维持这种降低。仅 PRO 和 KET+PRO 增加了 mTOR-Rheb 共定位;然而,在 KET+PRO 时,增加更为明显。处理摄入增加了 mTOR-WGA 共定位,提示向纤维外周转运。酮体影响 mTOR 的空间调节。
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