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急性运动通过重塑mRNA mA甲基化促进白色脂肪组织褐变。

Acute exercise promotes WAT browning by remodeling mRNA mA methylation.

作者信息

Chen Wei, Liu Youhua, Liu Jiaqi, Chen Yushi, Wang Xinxia

机构信息

College of Animal Sciences, Zhejiang University, Hangzhou 310058, China; Key Laboratory of Molecular Animal Nutrition (Zhejiang University), Ministry of Education, Key Laboratory of Animal Nutrition and Feed Science (Eastern of China), Ministry of Agriculture and Rural Affairs, Key Laboratory of Animal Feed and Nutrition of Zhejiang Province, Hangzhou 310058, China.

College of Animal Sciences, Zhejiang University, Hangzhou 310058, China; Key Laboratory of Molecular Animal Nutrition (Zhejiang University), Ministry of Education, Key Laboratory of Animal Nutrition and Feed Science (Eastern of China), Ministry of Agriculture and Rural Affairs, Key Laboratory of Animal Feed and Nutrition of Zhejiang Province, Hangzhou 310058, China.

出版信息

Life Sci. 2025 Jan 15;361:123269. doi: 10.1016/j.lfs.2024.123269. Epub 2024 Nov 22.

Abstract

AIMS

Regular exercise promotes the beiging and metabolic adaptations of white adipose tissue (WAT) through the cumulative transcriptional responses that occur after each exercise session. However, the effects of a single bout of acute exercise and the role of N-methyladenosine (mA) in these adaptations remain unclear. We aim to investigate this further.

MATERIALS AND METHODS

We constructed mouse models for chronic (8 weeks of running) and acute (single 1-hour run) exercise to study the effects on white adipose tissue (WAT) metabolism and beiging through metabolic phenotyping and transcriptome sequencing. Additionally, we explored the impact of acute exercise on WAT mA modification and target genes, combining mA regulators with cell models to elucidate the role of mA in WAT exercise adaptation.

KEY FINDINGS

Here, we reveal that upregulated mA modification after acute exercise induces the formation of glycolytic beige fat (g-beige fat) in WAT. Mechanistically, the metabolite β-hydroxybutyrate (BHBA) secreted after acute exercise upregulates mA modification in WAT. This enhances mA-dependent translation of the histone acetyltransferase CREBBP, promoting the transcription of key beiging genes by increasing chromatin accessibility. Pharmacologically elevating circulating BHBA mimics the metabolic response induced by acute exercise, upregulating mA modification and its downstream signals. Additionally, BHBA exhibits long-term effects, improving metabolic homeostasis in obesity by promoting thermogenesis in WAT.

SIGNIFICANCE

Our results reveal the role of metabolites in WAT metabolic adaptation through mA-mediated chromatin accessibility after acute exercise, providing a novel therapeutic target for regulating WAT metabolism from a nutritional epigenetics perspective.

摘要

目的

规律运动通过每次运动后累积的转录反应促进白色脂肪组织(WAT)的米色化和代谢适应。然而,单次急性运动的影响以及N-甲基腺苷(mA)在这些适应过程中的作用仍不清楚。我们旨在进一步研究这一点。

材料与方法

我们构建了慢性(8周跑步)和急性(单次1小时跑步)运动的小鼠模型,通过代谢表型分析和转录组测序研究对白色脂肪组织(WAT)代谢和米色化的影响。此外,我们结合mA调节剂与细胞模型,探讨急性运动对WAT mA修饰和靶基因的影响,以阐明mA在WAT运动适应中的作用。

主要发现

在此,我们揭示急性运动后上调的mA修饰诱导WAT中糖酵解米色脂肪(g-米色脂肪)的形成。机制上,急性运动后分泌的代谢物β-羟基丁酸(BHBA)上调WAT中的mA修饰。这增强了组蛋白乙酰转移酶CREBBP的mA依赖性翻译,通过增加染色质可及性促进关键米色化基因的转录。药理学上提高循环中的BHBA可模拟急性运动诱导的代谢反应,上调mA修饰及其下游信号。此外,BHBA具有长期效应,通过促进WAT中的产热改善肥胖中的代谢稳态。

意义

我们的结果揭示了急性运动后代谢物通过mA介导的染色质可及性在WAT代谢适应中的作用,从营养表观遗传学角度为调节WAT代谢提供了一个新的治疗靶点。

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