首页> 外文期刊>The Journal of Pharmacology and Experimental Therapeutics: Official Publication of the American Society for Pharmacology and Experimental Therapeutics >An Inhibitor of Casein Kinase I epsilon Induces Phase Delays in Circadian Rhythms under Free-Running and Entrained Conditions
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An Inhibitor of Casein Kinase I epsilon Induces Phase Delays in Circadian Rhythms under Free-Running and Entrained Conditions

机译:酪蛋白激酶Iε抑制剂在自由奔放和夹带条件下诱导昼夜节律的相位延迟

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Casein kinase I epsilon(CKI epsilon)is an essential component of the biological clock,phosphorylating PER proteins,and in doing so regulating their turnover and nuclear entry in oscillator cells of the suprachiasmatic nucleus(SCN).Although hereditary decreases in PER phosphorylation have been well characterized,little is known about the consequences of acute enzyme inhibition by pharmacological means.A novel reagent,4-[3-cyclohexyl-5-(4-fluoro-phenyl)-3H-imidazol-4-yl]-pyrimidin-2-ylamine(PF-670462),proved to be both a potent(IC50=7.7+-2.2 nM)and selective(>30-fold with respect to 42 additional kinases)inhibitor of CKI epsilon in isolated enzyme preparations;in transfected whole cell assays,it caused a concentration-related redistribution of nuclear versus cytosolic PER.When tested in free-running animals,50 mg/kg s.c.PF-670462 produced robust phase delays when dosed at circadian time(CT)9(-1.97+-0.17 h).Entrained rats dosed in normal light-dark(LD)and then released to constant darkness also experienced phase delays that were dose-and time of dosing-dependent.PF-670462 yielded only phase delays across the circadian cycle with the most sensitive time at CT12 when PER levels are near their peak in the SCN.Most importantly,these drug-induced phase delays persisted in animals entrained and maintained in LD throughout the entire experiment;re-entrainment to the prevailing LD required days in contrast to the rapid elimination of the drug(t_(1/2)=0.46+-0.04 h).Together,these results suggest that inhibition of CKI epsilon yields a perturbation of oscillator function that forestalls light as a zeitgeber,and they demonstrate that pharmacological tools such as PF-670462 may yield valuable insight into clock function.
机译:酪蛋白激酶I epsilon(CKI epsilon)是生物钟的重要组成部分,磷酸化PER蛋白,从而调节其营业额和核分裂进入视交叉上核(SCN)的振荡细胞。尽管PER磷酸化的遗传性降低充分表征,对通过药理学方法抑制急性酶的后果知之甚少。一种新型试剂4- [3-环己基-5-(4-氟-苯基)-3H-咪唑-4-基]-嘧啶-2 -ylamine(PF-670462),在分离的酶制剂中被证明是一种有效的CKI epsilon抑制剂(IC50 = 7.7 + -2.2 nM)和选择性(相对于42种其他激酶> 30倍)抑制剂;在转染的全细胞中在自由奔跑的动物中进行测试时,在昼夜节律(CT)9剂量下,50 mg / kg scPF-670462产生了强大的相位延迟(9)(-1.97 + -0.17) h)。以正常的明暗(LD)剂量将训练后的大鼠释放出恒定的暗度PF-670462在整个昼夜节律周期中仅发生相位延迟,而当PER水平接近SCN峰值时,CT12的敏感时间最为敏感。最重要的是,这些药物诱导的相延迟在整个实验中在被LD夹带并保持在LD中的动物中持续存在;与快速消除药物相反,重新夹带至主要LD需要几天(t_(1/2)= 0.46 + -0.04 h)。总之,这些结果表明,抑制CKIε会产生振荡功能的扰动,从而阻止光作为Zegegeber,并且它们表明药理学工具(例如PF-670462)可能会产生对时钟功能的有价值的见解。

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