甲状腺激素受体 beta(THRB)对成年雄性小鼠昼夜肝脂代谢的依赖性调节

Leonardo Vinicius Monteiro de Assis, Lisbeth Harder, Julica Inderhees, Olaf Jöhren, Jens Mittag, Henrik Oster
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摘要

甲状腺激素(THs)是全身能量代谢和平衡的关键调节因子。在肝脏中,高TH作用通过促进胆固醇和甘油三酯的转化来防止脂肪变性,其中甲状腺激素受体β(THRB)信号传导起着关键作用。本研究探讨了甲状腺激素受体β(THRB)作用与肝脏能量代谢的另一个关键调节因子--昼夜节律时钟--之间的潜在相互作用。在正常进食条件下对THRB缺陷(THRBKO)小鼠的肝脏转录组分析表明,THRB缺失的影响不大。时间转录组和脂质组分析发现,由于 THRB 缺乏,昼夜代谢节律发生了显著变化,导致胆固醇、三酰和二酰甘油以及脂肪酸水平升高,从而形成了一种促僵化状态。在体外促进脂肪变性的条件下,THRB 在肝细胞中的激动作用证实了这些发现。将 THRBKO 小鼠和诱导高或低 TH 作用的小鼠的转录组图谱进行整合,发现了一部分对 TH 有反应但对 THRB 不敏感的基因,这些基因与免疫过程有牵连。总之,我们的研究揭示了不同的 TH 相关信号在肝脏生理调控中复杂的时间依赖性相互作用,这为在脂肪肝疾病中采用时间药理学方法操纵 TH/THRB 提供了机会。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Thyroid hormone receptor beta (THRB) dependent regulation of diurnal hepatic lipid metabolism in adult male mice

Thyroid hormone receptor beta (THRB) dependent regulation of diurnal hepatic lipid metabolism in adult male mice
Thyroid hormones (THs) are critical regulators of systemic energy metabolism and homeostasis. In the liver, high TH action protects against steatosis by enhancing cholesterol and triglyceride turnover, with thyroid hormone receptor beta (THRB) signaling playing a pivotal role. This study probed the potential interaction between THRB action and another critical regulator of liver energy metabolism, the circadian clock. Liver transcriptome analysis of THRB deficient (THRBKO) mice under normal chow conditions revealed a modest impact of THRB deletion. Temporal transcriptome and lipidome profiling uncovered significant alterations in diurnal metabolic rhythms attributable to THRB deficiency pointing to a pro-steatotic state with elevated levels of cholesterol, tri- and diacylglycerides, and fatty acids. These findings were confirmed by THRB agonization in hepatocytes under steatosis-promoting conditions in vitro. Integration of transcriptome profiles from THRBKO mice and mice with induced high or low TH action identified a subset of TH responsive but THRB insensitive genes implicated in immune processes. In summary, our study reveals a complex time-of-day dependent interaction of different TH-related signals in the regulation of liver physiology indicating an opportunity for chronopharmacological approaches to TH/THRB manipulation in fatty liver diseases.
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