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From the Cover: A KaiC-associating SasA–RpaA two-component regulatory system as a major circadian timing mediator in cyanobacteria

机译:从封面开始:与KaiC相关的SasA–RpaA两组分调节系统是蓝细菌的主要昼夜节律介质。

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摘要

KaiA, KaiB, and KaiC clock proteins from cyanobacteria and ATP are sufficient to reconstitute the KaiC phosphorylation rhythm in vitro, whereas almost all gene promoters are under the control of the circadian clock. The mechanism by which the KaiC phosphorylation cycle drives global transcription rhythms is unknown. Here, we report that RpaA, a potential DNA-binding protein that acts as a cognate response regulator of the KaiC-interacting kinase SasA, mediates between KaiC phosphorylation and global transcription rhythms. Circadian transcription was severely attenuated in sasA (Synechococcus adaptive sensor A)- and rpaA (regulator of phycobilisome-associated)-mutant cells, and the phosphotransfer activity from SasA to RpaA changed dramatically depending on the circadian state of a coexisting Kai protein complex in vitro. We propose a model in which the SasA–RpaA two-component system mediates time signals from the enzymatic oscillator to drive genome-wide transcription rhythms in cyanobacteria. Moreover, our results indicate the presence of secondary output pathways from the clock to transcription control, suggesting that multiple pathways ensure a genome-wide circadian system.
机译:来自蓝细菌和ATP的KaiA,KaiB和KaiC时钟蛋白足以在体外重构KaiC磷酸化节奏,而几乎所有基因启动子都在昼夜节律的控制下。 KaiC磷酸化循环驱动整体转录节律的机制尚不清楚。在这里,我们报道RpaA,一种潜在的DNA结合蛋白,充当KaiC相互作用激酶SasA的同源响应调节剂,介导KaiC磷酸化和整体转录节奏之间。在sasA(Synechococcus自适应传感器A)和rpaA(与藻胆体相关的调节剂)突变细胞中,昼夜节律的转录严重减弱,并且从SasA到RpaA的磷酸转移活性根据体外共存的Kai蛋白复合物的昼夜节律状态而发生了显着变化。 。我们提出了一个模型,其中SasA–RpaA两组分系统介导来自酶促振荡器的时间信号,以驱动蓝细菌中的全基因组转录节奏。此外,我们的结果表明存在从时钟到转录控制的二级输出途径,这表明多种途径可确保全基因组昼夜节律系统。

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