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急性有氧运动表明,FAHFAs 可区分超重和正常体重跑步者的代谢组。

Acute aerobic exercise reveals that FAHFAs distinguish the metabolomes of overweight and normal-weight runners.

机构信息

Division of Molecular Medicine, Department of Medicine.

Bioinformatics and Computational Biology Program.

出版信息

JCI Insight. 2022 Apr 8;7(7):e158037. doi: 10.1172/jci.insight.158037.

Abstract

BackgroundResponses of the metabolome to acute aerobic exercise may predict maximum oxygen consumption (VO2max) and longer-term outcomes, including the development of diabetes and its complications.MethodsSerum samples were collected from overweight/obese trained (OWT) and normal-weight trained (NWT) runners prior to and immediately after a supervised 90-minute treadmill run at 60% VO2max (NWT = 14, OWT = 11) in a cross-sectional study. We applied a liquid chromatography high-resolution-mass spectrometry-based untargeted metabolomics platform to evaluate the effect of acute aerobic exercise on the serum metabolome.ResultsNWT and OWT metabolic profiles shared increased circulating acylcarnitines and free fatty acids (FFAs) with exercise, while intermediates of adenine metabolism, inosine, and hypoxanthine were strongly correlated with body fat percentage and VO2max. Untargeted metabolomics-guided follow-up quantitative lipidomic analysis revealed that baseline levels of fatty acid esters of hydroxy fatty acids (FAHFAs) were generally diminished in the OWT group. FAHFAs negatively correlated with visceral fat mass and HOMA-IR. Strikingly, a 4-fold decrease in FAHFAs was provoked by acute aerobic running in NWT participants, an effect that negatively correlated with circulating IL-6; these effects were not observed in the OWT group. Machine learning models based on a preexercise metabolite profile that included FAHFAs, FFAs, and adenine intermediates predicted VO2max.ConclusionThese findings in overweight human participants and healthy controls indicate that exercise-provoked changes in FAHFAs distinguish normal-weight from overweight participants and could predict VO2max. These results support the notion that FAHFAs could modulate the inflammatory response, fuel utilization, and insulin resistance.Trial registrationClinicalTrials.gov, NCT02150889.FundingNIH DK091538, AG069781, DK098203, TR000114, UL1TR002494.

摘要

背景

代谢物对急性有氧运动的反应可能预测最大摄氧量(VO2max)和更长期的结果,包括糖尿病及其并发症的发展。

方法

在一项横断面研究中,超重/肥胖训练组(OWT)和正常体重训练组(NWT)的跑步者在 60% VO2max 的监督下进行 90 分钟跑步机跑步前后,采集血清样本(NWT=14,OWT=11)。我们应用基于液相色谱-高分辨率质谱的非靶向代谢组学平台来评估急性有氧运动对血清代谢组的影响。

结果

NWT 和 OWT 的代谢谱与运动共享增加的循环酰基肉碱和游离脂肪酸(FFAs),而腺嘌呤代谢的中间产物肌苷和次黄嘌呤与体脂百分比和 VO2max 呈强烈相关。非靶向代谢组学指导的后续定量脂质组学分析显示,OWT 组的脂肪酸羟脂肪酸酯(FAHFAs)基线水平普遍降低。FAHFAs 与内脏脂肪量和 HOMA-IR 呈负相关。引人注目的是,NWT 参与者急性有氧运动后 FAHFAs 下降了 4 倍,这与循环 IL-6 呈负相关;而在 OWT 组中没有观察到这种效应。基于包括 FAHFAs、FFAs 和腺嘌呤中间产物的运动前代谢物谱的机器学习模型预测了 VO2max。

结论

在超重的人类参与者和健康对照组中,这些发现表明,FAHFAs 引起的运动变化可以区分正常体重和超重参与者,并可以预测 VO2max。这些结果支持 FAHFAs 可以调节炎症反应、燃料利用和胰岛素抵抗的观点。

试验注册

ClinicalTrials.gov,NCT02150889。

资金

NIH DK091538、AG069781、DK098203、TR000114、UL1TR002494。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9067/9057596/16944d0249da/jciinsight-7-158037-g123.jpg

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