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全基因组转录可塑性是细胞适应新挑战的基础。

Genome-wide transcriptional plasticity underlies cellular adaptation to novel challenge.

作者信息

Stern Shay, Dror Tali, Stolovicki Elad, Brenner Naama, Braun Erez

机构信息

Department of Chemical Engineering, Technion-Israel Institute of Technology, Haifa, Israel.

出版信息

Mol Syst Biol. 2007;3:106. doi: 10.1038/msb4100147. Epub 2007 Apr 24.

Abstract

Cells adjust their transcriptional state to accommodate environmental and genetic perturbations. An open question is to what extent transcriptional response to perturbations has been specifically selected along evolution. To test the possibility that transcriptional reprogramming does not need to be 'pre-designed' to lead to an adaptive metabolic state on physiological timescales, we confronted yeast cells with a novel challenge they had not previously encountered. We rewired the genome by recruiting an essential gene, HIS3, from the histidine biosynthesis pathway to a foreign regulatory system, the GAL network responsible for galactose utilization. Switching medium to glucose in a chemostat caused repression of the essential gene and presented the cells with a severe challenge to which they adapted over approximately 10 generations. Using genome-wide expression arrays, we show here that a global transcriptional reprogramming (>1200 genes) underlies the adaptation. A large fraction of the responding genes is nonreproducible in repeated experiments. These results show that a nonspecific transcriptional response reflecting the natural plasticity of the regulatory network supports adaptation of cells to novel challenges.

摘要

细胞会调整其转录状态以适应环境和基因扰动。一个悬而未决的问题是,在进化过程中,转录对扰动的反应在多大程度上经过了专门选择。为了测试转录重编程无需“预先设计”就能在生理时间尺度上导致适应性代谢状态的可能性,我们让酵母细胞面临一种它们以前从未遇到过的新挑战。我们通过将一个必需基因HIS3从组氨酸生物合成途径招募到一个外来调控系统(负责半乳糖利用的GAL网络)来重新连接基因组。在恒化器中将培养基换成葡萄糖会导致必需基因受到抑制,并给细胞带来严峻挑战,它们在大约10代的时间里适应了这一挑战。我们在这里使用全基因组表达阵列表明,全局转录重编程(>1200个基因)是适应的基础。在重复实验中,很大一部分响应基因是不可重复的。这些结果表明,反映调控网络自然可塑性的非特异性转录反应支持细胞适应新挑战。

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