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Model-based investigation of the circadian clock and cell cycle coupling in mouse embryonic fibroblasts: Prediction of RevErb-alpha up-regulation during mitosis

机译:小鼠胚胎成纤维细胞中昼夜节律和细胞周期偶联的基于模型的研究:有丝分裂期间RevErb-α上调的预测

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Experimental observations have put in evidence autonomous self-sustained circadian oscillators in most mammalian cells, and proved the existence of molecular links between the circadian clock and the cell cycle. Some mathematical models have also been built to assess conditions of control of the cell cycle by the circadian clock. However, recent studies in individual NIH3T3 fibroblasts have shown an unexpected acceleration of the circadian clock together with the cell cycle when the culture medium is enriched with growth factors, and the absence of such acceleration in confluent cells. In order to explain these observations, we study a possible entrainment of the circadian clock by the cell cycle through a regulation of clock genes around the mitosis phase. We develop a computational model and a formal specification of the observed behavior to investigate the conditions of entrainment in period and phase. We show that either the selective activation of RevErb-alpha or the selective inhibition of Bmal1 transcription during the mitosis phase, allow us to fit the experimental data on both period and phase, while a uniform inhibition of transcription during mitosis seems incompatible with the phase data. We conclude on the arguments favoring the RevErb-alpha up-regulation hypothesis and on some further predictions of the model. (C) 2016 Elsevier Ireland Ltd. All rights reserved.
机译:实验观察表明,在大多数哺乳动物细胞中自主自我维持的生物钟振荡器,并证明了生物钟和细胞周期之间存在分子联系。还建立了一些数学模型来评估由生物钟控制细胞周期的条件。但是,最近对单个NIH3T3成纤维细胞的研究表明,当培养基中富含生长因子时,昼夜节律的出现会伴随细胞周期的意外加速,而在融合细胞中则不会出现这种加速。为了解释这些观察结果,我们研究了通过调控有丝分裂期周围时钟基因的细胞周期对昼夜节律的夹带。我们开发了一个计算模型和观察到的行为的形式规范,以调查时期和阶段的夹带条件。我们表明,在有丝分裂阶段选择性激活RevErb-alpha或选择性抑制Bmal1转录,可以使我们在周期和阶段上均拟合实验数据,而在有丝分裂期间对转录的统一抑制似乎与该阶段数据不兼容。 。我们得出了支持RevErb-alpha上调假设的论据以及对该模型的一些进一步预测的结论。 (C)2016 Elsevier Ireland Ltd.保留所有权利。

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