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Theoretical Analysis of Competing Conformational Transitions in Superhelical DNA

机译:超螺旋DNA竞争构象转变的理论分析

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摘要

We develop a statistical mechanical model to analyze the competitive behavior of transitions to multiple alternate conformations in a negatively supercoiled DNA molecule of kilobase length and specified base sequence. Since DNA superhelicity topologically couples together the transition behaviors of all base pairs, a unified model is required to analyze all the transitions to which the DNA sequence is susceptible. Here we present a first model of this type. Our numerical approach generalizes the strategy of previously developed algorithms, which studied superhelical transitions to a single alternate conformation. We apply our multi-state model to study the competition between strand separation and B-Z transitions in superhelical DNA. We show this competition to be highly sensitive to temperature and to the imposed level of supercoiling. Comparison of our results with experimental data shows that, when the energetics appropriate to the experimental conditions are used, the competition between these two transitions is accurately captured by our algorithm. We analyze the superhelical competition between B-Z transitions and denaturation around the c-myc oncogene, where both transitions are known to occur when this gene is transcribing. We apply our model to explore the correlation between stress-induced transitions and transcriptional activity in various organisms. In higher eukaryotes we find a strong enhancement of Z-forming regions immediately 5′ to their transcription start sites (TSS), and a depletion of strand separating sites in a broad region around the TSS. The opposite patterns occur around transcript end locations. We also show that susceptibility to each type of transition is different in eukaryotes and prokaryotes. By analyzing a set of untranscribed pseudogenes we show that the Z-susceptibility just downstream of the TSS is not preserved, suggesting it may be under selection pressure.
机译:我们开发了一个统计力学模型,以分析在千碱基长和特定碱基序列的负超螺旋DNA分子中过渡到多种交替构象的竞争行为。由于DNA超螺旋性在拓扑上将所有碱基对的跃迁行为耦合在一起,因此需要一个统一的模型来分析DNA序列易感的所有跃迁。在这里,我们介绍这种类型的第一个模型。我们的数值方法概括了以前开发的算法的策略,该算法研究了超螺旋转变为单个替代构象的情况。我们应用我们的多状态模型研究超螺旋DNA中链分离与B-Z跃迁之间的竞争。我们证明了这种竞争对温度和强加的超螺旋高度敏感。我们的结果与实验数据的比较表明,当使用适合实验条件的能量时,我们的算法可以准确地捕获这两个转变之间的竞争。我们分析了B-Z转变与c-myc癌基因周围变性之间的超螺旋竞争,已知该基因转录时两个转变都发生。我们应用我们的模型来探索各种生物在压力诱导的过渡和转录活性之间的相关性。在高等真核生物中,我们发现紧靠其转录起始位点(TSS)5'的Z形成区的强力增强,以及围绕TSS的宽阔区域中链分离位点的耗尽。相反的模式发生在转录本末端位置附近。我们还表明,在真核生物和原核生物中,每种过渡类型的敏感性都不同。通过分析一组未转录的假基因,我们表明未保留TSS下游的Z敏感性,这表明它可能处于选择压力下。

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