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The transcription factor Cabut coordinates energy metabolism and the circadian clock in response to sugar sensing

机译:转录因子Cabut响应糖分感应协调能量代谢和生物钟

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摘要

Nutrient sensing pathways adjust metabolism and physiological functions in response to food intake. For example, sugar feeding promotes lipogenesis by activating glycolytic and lipogenic genes through the Mondo/ChREBP-Mlx transcription factor complex. Concomitantly, other metabolic routes are inhibited, but the mechanisms of transcriptional repression upon sugar sensing have remained elusive. Here, we characterize cabut (cbt), a transcription factor responsible for the repressive branch of the sugar sensing transcriptional network in Drosophila. We demonstrate that cbt is rapidly induced upon sugar feeding through direct regulation by Mondo-Mlx. We found that CBT represses several metabolic targets in response to sugar feeding, including both isoforms of phosphoenolpyruvate carboxykinase (pepck). Deregulation of pepck1 (CG17725) in mlx mutants underlies imbalance of glycerol and glucose metabolism as well as developmental lethality. Furthermore, we demonstrate that cbt provides a regulatory link between nutrient sensing and the circadian clock. Specifically, we show that a subset of genes regulated by the circadian clock are also targets of CBT. Moreover, perturbation of CBT levels leads to deregulation of the circadian transcriptome and circadian behavioral patterns.
机译:营养感应途径可根据食物摄入量调节新陈代谢和生理功能。例如,通过Mondo / ChREBP-Mlx转录因子复合物激活糖酵解和脂肪生成基因,进食糖可以促进脂肪生成。伴随地,其他代谢途径被抑制,但是糖感测时的转录抑制机制仍然难以捉摸。在这里,我们表征cabut(cbt),果蝇中负责糖感测转录网络的阻抑分支的转录因子。我们证明cbt是通过Mondo-Mlx的直接调节在食糖后迅速诱导的。我们发现CBT抑制了对糖的摄食,包括磷酸烯醇丙酮酸羧化激酶(pepck)的两种同工型响应的几个代谢目标。 mlx突变体中pepck1(CG17725)的失调是甘油和葡萄糖代谢失衡以及发育杀伤力的基础。此外,我们证明cbt提供了营养素感测与生物钟之间的调节联系。具体而言,我们表明由昼夜节律调节的基因的子集也是CBT的目标。而且,CBT水平的扰动导致昼夜节律转录组和昼夜节律行为模式的失调。

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