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Dynamics of oscillatory phenotypes in S. cerevisiae reveal a network of genome-wide transcriptional oscillators

机译:酿酒酵母振荡表型的动态揭示了一种基因组转录振荡器网络

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摘要

Genetic and environmental factors are well-studied influences on phenotype; however, time is a variable that is rarely considered when studying changes in cellular phenotype. Time-resolved microarray data revealed genome-wide transcriptional oscillation in a yeast continuous culture system with ~2 and ~4 h periods. We mapped the global patterns of transcriptional oscillations into a 3D map to represent different cellular phenotypes of redox cycles. This map shows the dynamic nature of gene expression in that transcripts are ordered and coupled to each other through time and concentration space. Although cells differed in oscillation periods, transcripts involved in certain processes were conserved in a deterministic way. When oscillation period lengthened, the peak to trough ratio of transcripts increased and the fraction of cells in the unbudded (G0/G1) phase of the cell division cycle increased. Decreasing the glucose level in the culture media was one way to increase the redox cycle, possibly from changes in metabolic flux. The period may be responding to lower glucose levels by increasing the fraction of cells in G1 and reducing S-phase gating so that cells can spend more time in catabolic processes. Our results support that gene transcripts are coordinated with metabolic functions and the cell division cycle.
机译:遗传和环境因素是研究表型的良好影响;然而,时间是在研究细胞表型的变化时很少考虑的变量。时间分辨的微阵列数据揭示了酵母连续培养系统中的基因组转录振荡,〜2和〜4小时。我们将转录振荡的全局模式映射到3D地图中,以表示氧化还原循环的不同细胞表型。该地图显示了通过时间和浓度空间彼此排序并耦合的基因表达的动态性质。虽然细胞在振荡周期中不同,但在某些过程中涉及的转录物以确定性的方式保守。当振荡周期延长时,转录物的峰与细胞分裂周期的不熟悉(G0 / G1)相中的细胞的级分增加。减少培养基中的葡萄糖水平是增加氧化还原循环的一种方法,可能来自代谢通量的变化。通过增加G1中的细胞的级分和还原S相衔接来响应降低葡萄糖水平,使得细胞可以在分解代谢过程中花费更多时间。我们的研究结果支持基因转录物与代谢功能和细胞分裂周期协调。

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