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Combinatorial gene regulation by modulation of relative pulse timing

机译:通过调节相对脉冲时间来调节组合基因

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摘要

Studies of individual living cells have revealed that many transcription factors activate in dynamic, and often stochastic, pulses within the same cell. However, it has remained unclear whether cells might exploit the dynamic interaction of these pulses to control gene expression. Here, using quantitative single-cell time-lapse imaging of Saccharomyces cerevisiae, we show that the pulsatile transcription factors Msn2 and Mig1 combinatorially regulate their target genes through modulation of their relative pulse timing. The activator Msn2 and repressor Mig1 showed pulsed activation in either a temporally overlapping or non-overlapping manner during their transient response to different inputs, with only the non-overlapping dynamics efficiently activating target gene expression. Similarly, under constant environmental conditions, where Msn2 and Mig1 exhibit sporadic pulsing, glucose concentration modulated the temporal overlap between pulses of the two factors. Together, these results reveal a time-based mode of combinatorial gene regulation. Regulation through relative signal timing is common in engineering and neurobiology, and these results suggest that it could also function broadly within the signalling and regulatory systems of the cell.
机译:对单个活细胞的研究表明,许多转录因子在同一细胞内以动态脉冲(通常是随机脉冲)激活。然而,目前尚不清楚细胞是否可以利用这些脉冲的动态相互作用来控制基因表达。在这里,使用酿酒酵母的定量单细胞延时成像,我们表明脉动转录因子Msn2和Mig1通过调节其相对脉冲时间组合地调节其靶基因。激活子Msn2和阻遏子Mig1在对不同输入的瞬态响应过程中以时间重叠或不重叠的方式显示了脉冲激活,只有不重叠的动力学有效地激活了目标基因的表达。同样,在恒定的环境条件下,Msn2和Mig1出现零星的脉动,葡萄糖浓度调节了这两个因素的脉冲之间的时间重叠。总之,这些结果揭示了组合基因调控的基于时间的模式。通过相对信号定时进行调节在工程和神经生物学中很常见,这些结果表明,它也可以在细胞的信号和调节系统中广泛发挥作用。

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