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真实序列对转录因子在DNA上搜索动力学的影响。

Real sequence effects on the search dynamics of transcription factors on DNA.

作者信息

Bauer Maximilian, Rasmussen Emil S, Lomholt Michael A, Metzler Ralf

机构信息

1] Institute for Physics &Astronomy, University of Potsdam, 14476 Potsdam-Golm, Germany [2] Department of Physics, Technical University of Munich, 85747 Garching Germany.

MEMPHYS-Centre for Biomembrane Physics, Department of Physics, Chemistry, and Pharmacy, University of Southern Denmark, Odense, Denmark.

出版信息

Sci Rep. 2015 Jul 8;5:10072. doi: 10.1038/srep10072.

Abstract

Recent experiments show that transcription factors (TFs) indeed use the facilitated diffusion mechanism to locate their target sequences on DNA in living bacteria cells: TFs alternate between sliding motion along DNA and relocation events through the cytoplasm. From simulations and theoretical analysis we study the TF-sliding motion for a large section of the DNA-sequence of a common E. coli strain, based on the two-state TF-model with a fast-sliding search state and a recognition state enabling target detection. For the probability to detect the target before dissociating from DNA the TF-search times self-consistently depend heavily on whether or not an auxiliary operator (an accessible sequence similar to the main operator) is present in the genome section. Importantly, within our model the extent to which the interconversion rates between search and recognition states depend on the underlying nucleotide sequence is varied. A moderate dependence maximises the capability to distinguish between the main operator and similar sequences. Moreover, these auxiliary operators serve as starting points for DNA looping with the main operator, yielding a spectrum of target detection times spanning several orders of magnitude. Auxiliary operators are shown to act as funnels facilitating target detection by TFs.

摘要

最近的实验表明,转录因子(TFs)确实利用易化扩散机制在活细菌细胞的DNA上定位其靶序列:TFs在沿DNA的滑动运动和通过细胞质的重新定位事件之间交替。通过模拟和理论分析,我们基于具有快速滑动搜索状态和能够进行靶标检测的识别状态的双态TF模型,研究了常见大肠杆菌菌株一大段DNA序列上的TF滑动运动。对于在从DNA解离之前检测到靶标的概率,TF搜索时间自洽地严重依赖于基因组区域中是否存在辅助操纵子(与主要操纵子相似的可及序列)。重要的是,在我们的模型中,搜索状态和识别状态之间的相互转化率对基础核苷酸序列的依赖程度是变化的。适度的依赖性使区分主要操纵子和相似序列的能力最大化。此外,这些辅助操纵子作为与主要操纵子进行DNA环化的起始点,产生了跨越几个数量级的一系列靶标检测时间。辅助操纵子被证明起到促进TFs进行靶标检测的漏斗作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8753/5507490/e0fd650e77c2/srep10072-f1.jpg

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