PURPOSE: Nutritional ketosis is purported to enhance skeletal muscle recovery and adaptation to exercise, yet precise adaptive mechanisms are unknown. We investigated the post-exercise molecular response to ketone monoesters (KME) in skeletal muscle by characterising the early transcriptomic response. METHODS: Following a randomised, double-blind, crossover design, recreationally active men (nâ=â9, age: 26â±â5 (meansâ±âSD) y; VÌO(2max): 47â±â4 mL·kg(-1)·min(-1)) completed two experimental trials where they ingested either 1.25 g·kg(-1) of KME or a taste-matched placebo (PLA) drink during exercise (90-min cycling at 60% of VÌO(2max)) and 3-h recovery. Blood samples were taken throughout for hormone and metabolite analyses, and muscle biopsies were taken at baseline and 3 h post-exercise for glycogen and genome-wide gene expression analyses. RESULTS: Recovery ÃHB concentrations were higher in KME (4.1â±â0.7 mM) vs PLA (0.1â±â0.0 mM, Pâ<â0.001). Erythropoietin (EPO) showed a main effect of time (Pâ=â0.044), but no condition effect (Pâ=â0.087) or interaction (Pâ=â0.318). Skeletal muscle glycogen decreased post-exercise (-57%, Pâ<â0.001) as expected, but showed no condition effect (Pâ=â0.889) or interaction (Pâ=â0.907). We measured the expression of 16,898 genes, and despite a clear time effect on the skeletal muscle transcriptome (1561 differentially expressed genes post vs pre-exercise; qâ<â0.05 fold changeâ>â±â1.5), there was no effect of condition. CONCLUSIONS: KME did not demonstrate an effect on EPO concentration, muscle glycogen or transcriptome, suggesting DNA translation is likely not a process directly regulated by acute ketonaemia that increases early post-exercise.
Acute nutritional ketosis during early recovery from aerobic exercise does not affect skeletal muscle transcriptomic response in humans.
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作者:Mosquera-Lopez Erick, Louis Julien, Edwards Jason P, Pugh Jamie, Viggars Mark R, Owens Daniel J, Areta Jose L
| 期刊: | European Journal of Applied Physiology | 影响因子: | 2.700 |
| 时间: | 2026 | 起止号: | 2026 Feb;126(2):1021-1032 |
| doi: | 10.1007/s00421-025-05987-9 | ||
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