Melatonin restores hepatic lipid metabolic homeostasis disrupted by blue light at night in high-fat diet-fed mice

IF 8.3 1区 医学 Q1 ENDOCRINOLOGY & METABOLISM
Qingyun Guan, Zixu Wang, Jing Cao, Yulan Dong, Shusheng Tang, Yaoxing Chen
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Abstract

Artificial light at night (ALAN) is an emerging environmental pollutant that threatens public health. Recently, ALAN has been identified as a risk factor for obesity; however, the role of ALAN and its light wavelength in hepatic lipid metabolic homeostasis remains undetermined. We showed that chronic dim (~5 lx) ALAN (dLAN) exposure significantly promoted hepatic lipid accumulation in obese or diabetic mice, with the most severe effect of blue light and little effect of green or red light. These metabolic phenotypes were attributed to blue rather than green or red dLAN interfering with hepatic lipid metabolism, especially lipogenesis and lipolysis. Further studies found that blue dLAN disrupted hepatic lipogenesis and lipolysis processes by inhibiting hepatic REV-ERBs. Mechanistically, feeding behavior mediated the regulation of dLAN on hepatic REV-ERBs. In addition, different effects of light wavelengths at night on liver REV-ERBs depended on the activation of the corticosterone (CORT)/glucocorticoid receptor (GR) axis. Blue dLAN could activate the CORT/GR axis significantly while other wavelengths could not. Notably, we demonstrated that exogenous melatonin could effectively inhibit hepatic lipid accumulation and restore the hepatic GR/REV-ERBs axis disrupted by blue dLAN. These findings demonstrate that dLAN promotes hepatic lipid accumulation in mice via a short-wavelength-dependent manner, and exogenous melatonin is a potential therapeutic approach. This study strengthens the relationship between ALAN and hepatic lipid metabolism and provides insights into directing ambient light.

褪黑素可恢复高脂饮食小鼠夜间被蓝光破坏的肝脏脂质代谢平衡。
夜间人造光(ALAN)是一种威胁公众健康的新兴环境污染物。最近,ALAN 被确定为肥胖症的一个风险因素;然而,ALAN 及其光波长在肝脏脂质代谢平衡中的作用仍未确定。我们的研究表明,长期暴露于暗光(约 5 lx)ALAN(dLAN)会显著促进肥胖或糖尿病小鼠肝脏脂质的积累,其中蓝光的影响最为严重,而绿光或红光的影响很小。这些代谢表型归因于蓝色而非绿色或红色 dLAN 干扰了肝脏脂质代谢,尤其是脂肪生成和脂肪分解。进一步研究发现,蓝色 dLAN 通过抑制肝脏 REV-ERBs 干扰了肝脏脂肪生成和脂肪分解过程。从机理上讲,摄食行为介导了dLAN对肝脏REV-ERBs的调节。此外,夜间光波长对肝脏REV-ERB的不同影响取决于皮质酮(CORT)/糖皮质激素受体(GR)轴的激活。蓝色 dLAN 能显著激活 CORT/GR 轴,而其他波长则不能。值得注意的是,我们证明外源性褪黑素能有效抑制肝脏脂质积累,并恢复被蓝色 dLAN 破坏的肝脏 GR/REV-ERBs 轴。这些研究结果表明,dLAN 通过短波长依赖性方式促进小鼠肝脏脂质积累,而外源性褪黑激素是一种潜在的治疗方法。这项研究加强了 ALAN 与肝脏脂质代谢之间的关系,并为引导环境光提供了启示。
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来源期刊
Journal of Pineal Research
Journal of Pineal Research 医学-内分泌学与代谢
CiteScore
17.70
自引率
4.90%
发文量
66
审稿时长
1 months
期刊介绍: The Journal of Pineal Research welcomes original scientific research on the pineal gland and melatonin in vertebrates, as well as the biological functions of melatonin in non-vertebrates, plants, and microorganisms. Criteria for publication include scientific importance, novelty, timeliness, and clarity of presentation. The journal considers experimental data that challenge current thinking and welcomes case reports contributing to understanding the pineal gland and melatonin research. Its aim is to serve researchers in all disciplines related to the pineal gland and melatonin.
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