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Translational control of entrainment and synchrony of the suprachiasmatic circadian clock by mTOR/4E-BP1 signaling

机译:mTOR / 4E-BP1信号对平视上生物钟的夹带和同步的平移控制

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摘要

Protein synthesis is critical for circadian clock function, but little is known of how translational regulationcontrols the master pacemaker in mammals, the suprachiasmatic nucleus (SCN). Here we demonstrate that the pivotal translational repressor, the eukaryotic translational initiation factor 4E binding protein 1 (4E-BP1), is rhythmically regulated via the mechanistic target of rapamycin (mTOR) signaling in the SCN and preferentially represses vasoactive intestinal peptide (Vip) mRNA translation. Knockout (KO) of Eif4ebp1 (gene encoding 4E-BP1) leads to upregulation of VIP and higher amplitude of molecular rhythms in the SCN. Consequently, the 4E-BP1 null mice exhibit accelerated re-entrainment to a shifted light/dark cycle and are more resistant to the rhythm-disruptive effects of constant light. Conversely, in Mtor+/- mice VIP expression is decreased and susceptibility to the effects of constant light is increased. These results reveal a key role for mTOR/4E-BP1-mediated translational control in regulating entrainment and synchrony of the master clock.
机译:蛋白质合成对于昼夜节律功能至关重要,但对于翻译调控如何控制哺乳动物的上交叉眼核(SCN)的了解很少。在这里,我们证明了枢轴翻译阻遏物,真核翻译起始因子4E结合蛋白1(4E-BP1),通过SCN中雷帕霉素(mTOR)信号转导的机制靶点有节奏地调控,并优先抑制血管活性肠肽(Vip)mRNA翻译。 Eif4ebp1(编码4E-BP1的基因)的敲除(KO)导致VIP的上调和SCN中更高的分子节律幅度。因此,空4E-BP1小鼠表现出加速的重新夹带,以改变光/暗周期,并且对恒定光的节律性破坏作用更有抵抗力。相反,在Mtor +/-小鼠中,VIP表达降低,并且对持续光照的敏感性增加。这些结果揭示了mTOR / 4E-BP1介导的翻译控制在调节主时钟的夹带和同步中的关键作用。

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