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通过单分子噪声分析揭示转录因子的随机表达动力学。

Stochastic expression dynamics of a transcription factor revealed by single-molecule noise analysis.

机构信息

Department of Biophysics and Biophysical Chemistry, Johns Hopkins University School of Medicine, Baltimore, Maryland, USA.

出版信息

Nat Struct Mol Biol. 2012 Aug;19(8):797-802. doi: 10.1038/nsmb.2336. Epub 2012 Jul 1.

Abstract

Gene expression is inherently stochastic; precise gene regulation by transcription factors is important for cell-fate determination. Many transcription factors regulate their own expression, suggesting that autoregulation counters intrinsic stochasticity in gene expression. Using a new strategy, cotranslational activation by cleavage (CoTrAC), we probed the stochastic expression dynamics of cI, which encodes the bacteriophage λ repressor CI, a fate-determining transcription factor. CI concentration fluctuations influence both lysogenic stability and induction of bacteriophage λ. We found that the intrinsic stochasticity in cI expression was largely determined by CI expression level irrespective of autoregulation. Furthermore, extrinsic, cell-to-cell variation was primarily responsible for CI concentration fluctuations, and negative autoregulation minimized CI concentration heterogeneity by counteracting extrinsic noise and introducing memory. This quantitative study of transcription factor expression dynamics sheds light on the mechanisms cells use to control noise in gene regulatory networks.

摘要

基因表达本质上是随机的;转录因子对基因的精确调控对于细胞命运的决定至关重要。许多转录因子调节自身的表达,这表明自我调节可以抵消基因表达中的内在随机性。使用一种新的策略,翻译共激活(CoTrAC),我们探测了编码噬菌体 λ 阻遏物 CI 的 cI 的随机表达动力学,CI 是一个决定命运的转录因子。CI 浓度波动既影响溶原稳定性,也影响噬菌体 λ 的诱导。我们发现,cI 表达的内在随机性主要由 CI 表达水平决定,而与自我调节无关。此外,细胞间的外在变异性是 CI 浓度波动的主要原因,负自我调节通过抵消外在噪声和引入记忆最小化 CI 浓度异质性。这项关于转录因子表达动力学的定量研究揭示了细胞用于控制基因调控网络中噪声的机制。

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