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Mini Screening of Kinase Inhibitors Affecting Period-length of Mammalian Cellular Circadian Clock

机译:影响哺乳动物细胞昼夜节律时钟周期长度的激酶抑制剂的微型筛选。

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摘要

In mammalian circadian rhythms, the transcriptional-translational feedback loop (TTFL) consisting of a set of clock genes is believed to elicit the circadian clock oscillation. The TTFL model explains that the accumulation and degradation of mPER and mCRY proteins control the period-length (tau) of the circadian clock. Although recent studies revealed that the Casein Kinase Iεδ (CKIεδ) regurates the phosphorylation of mPER proteins and the circadian period-length, other kinases are also likely to contribute the phosphorylation of mPER. Here, we performed small scale screening using 84 chemical compounds known as kinase inhibitors to identify candidates possibly affecting the circadian period-length in mammalian cells. Screening by this high-throughput real-time bioluminescence monitoring system revealed that the several chemical compounds apparently lengthened the cellular circadian clock oscillation. These compounds are known as inhibitors against kinases such as Casein Kinase II (CKII), PI3-kinase (PI3K) and c-Jun N-terminal Kinase (JNK) in addition to CKIεδ. Although these kinase inhibitors may have some non-specific effects on other factors, our mini screening identified new candidates contributing to period-length control in mammalian cells.
机译:在哺乳动物昼夜节律中,由一组时钟基因组成的转录-翻译反馈环(TTFL)被认为引起了昼夜节律振荡。 TTFL模型解释了mPER和mCRY蛋白的积累和降解控制了生物钟的周期长度(tau)。尽管最近的研究表明酪蛋白激酶Iεδ(CKIεδ)调节了mPER蛋白的磷酸化和昼夜节律周期长度,但其他激酶也可能有助于mPER的磷酸化。在这里,我们使用84种化合物(称为激酶抑制剂)进行了小规模筛选,以确定可能影响哺乳动物细胞中昼夜节律周期长度的候选物。通过这种高通量实时生物发光监测系统进行的筛选显示,几种化合物显然延长了细胞生物钟的振荡。这些化合物除CKIεδ外,还被称为激酶的抑制剂,如酪蛋白激酶II(CKII),PI3-激酶(PI3K)和c-Jun N末端激酶(JNK)。尽管这些激酶抑制剂可能对其他因素有一些非特异性作用,但我们的小型筛查发现了有助于哺乳动物细胞周期控制的新候选药物。

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