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Pharmacological modulation of circadian rhythms by synthetic activators of the deacetylase SIRT1

机译:脱乙酰基酶SIRT1的合成激活剂对昼夜节律的药理调节

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摘要

Circadian rhythms govern a wide variety of physiological and metabolic functions in many organisms, from prokaryotes to humans. We previously reported that silent information regulator 1 (SIRT1), a NAD+-dependent deacetylase, contributes to circadian control. In addition, SIRT1 activity is regulated in a cyclic manner in virtue of the circadian oscillation of the coenzyme NAD+. Here we used specific SIRT1 activator compounds both in vitro and in vivo. We tested a variety of compounds to show that the activation of SIRT1 alters CLOCK:BMAL1-driven transcription in different systems. Activation of SIRT1 induces repression of circadian gene expression and decreases H3 K9/K14 acetylation at corresponding promoters in a time-specific manner. Specific activation of SIRT1 was demonstrated in vivo using liver-specific SIRT1-deficient mice, where the effect of SIRT1 activator compounds was shown to be dependent on SIRT1. Our findings demonstrate that SIRT1 can fine-tune circadian rhythm and pave the way to the development of pharmacological strategies to address a broad range of therapeutic indications.
机译:从原核生物到人类,昼夜节律控制着许多生物体的多种生理和代谢功能。我们先前曾报道,沉默信息调节因子1(SIRT1)是NAD + 依赖性脱乙酰基酶,有助于昼夜节律的控制。另外,借助于辅酶NAD + 的昼夜节律振荡,SIRT1活性以循环方式被调节。在这里,我们在体外和体内都使用了特定的SIRT1激活剂化合物。我们测试了多种化合物,以显示SIRT1的激活在不同系统中改变了CLOCK:BMAL1驱动的转录。 SIRT1的激活诱导昼夜节律基因表达的抑制,并以时间特异性方式降低相应启动子处的H3 K9 / K14乙酰化。使用肝特异性SIRT1缺陷小鼠在体内证明了SIRT1的特异性激活,其中SIRT1激活剂化合物的作用被证明依赖于SIRT1。我们的发现表明,SIRT1可以调节昼夜节律,并为解决广泛的治疗适应症的药理策略的发展铺平道路。

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