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超螺旋 DNA 中应力诱导的 B-Z 转变的理论分析。

Theoretical analysis of the stress induced B-Z transition in superhelical DNA.

机构信息

UC Davis Genome Center, University of California, Davis, Davis California, United States of America.

出版信息

PLoS Comput Biol. 2011 Jan 20;7(1):e1001051. doi: 10.1371/journal.pcbi.1001051.

Abstract

We present a method to calculate the propensities of regions within a DNA molecule to transition from B-form to Z-form under negative superhelical stresses. We use statistical mechanics to analyze the competition that occurs among all susceptible Z-forming regions at thermodynamic equilibrium in a superhelically stressed DNA of specified sequence. This method, which we call SIBZ, is similar to the SIDD algorithm that was previously developed to analyze superhelical duplex destabilization. A state of the system is determined by assigning to each base pair either the B- or the Z-conformation, accounting for the dinucleotide repeat unit of Z-DNA. The free energy of a state is comprised of the nucleation energy, the sequence-dependent B-Z transition energy, and the energy associated with the residual superhelicity remaining after the change of twist due to transition. Using this information, SIBZ calculates the equilibrium B-Z transition probability of each base pair in the sequence. This can be done at any physiologically reasonable level of negative superhelicity. We use SIBZ to analyze a variety of representative genomic DNA sequences. We show that the dominant Z-DNA forming regions in a sequence can compete in highly complex ways as the superhelicity level changes. Despite having no tunable parameters, the predictions of SIBZ agree precisely with experimental results, both for the onset of transition in plasmids containing introduced Z-forming sequences and for the locations of Z-forming regions in genomic sequences. We calculate the transition profiles of 5 kb regions taken from each of 12,841 mouse genes and centered on the transcription start site (TSS). We find a substantial increase in the frequency of Z-forming regions immediately upstream from the TSS. The approach developed here has the potential to illuminate the occurrence of Z-form regions in vivo, and the possible roles this transition may play in biological processes.

摘要

我们提出了一种计算 DNA 分子中区域从 B 型向 Z 型转变倾向的方法,该方法适用于在负超螺旋应变下。我们使用统计力学来分析在指定序列的超螺旋应变 DNA 中,热力学平衡时所有易感 Z 形成区域之间发生的竞争。这种方法,我们称之为 SIBZ,与之前开发的用于分析超螺旋双螺旋体失稳的 SIDD 算法相似。系统的状态通过为每个碱基对分配 B 或 Z 构象来确定,考虑到 Z-DNA 的二核苷酸重复单元。状态的自由能由成核能、序列依赖性 B-Z 转变能以及由于转变导致扭转变化后剩余超螺旋能组成。利用这些信息,SIBZ 计算序列中每个碱基对的平衡 B-Z 转变概率。这可以在任何生理上合理的负超螺旋水平下完成。我们使用 SIBZ 分析了各种有代表性的基因组 DNA 序列。我们表明,在超螺旋水平变化时,序列中占主导地位的 Z-DNA 形成区域可以以非常复杂的方式竞争。尽管没有可调参数,但 SIBZ 的预测与实验结果完全一致,无论是在含有引入 Z 形成序列的质粒中的转变开始,还是在基因组序列中的 Z 形成区域的位置。我们计算了从 12841 个小鼠基因中的每一个的 5kb 区域的转变分布,并以转录起始位点(TSS)为中心。我们发现,在 TSS 上游的 Z 形成区域的频率显著增加。这里开发的方法有可能阐明体内 Z 形成区域的发生情况,以及这种转变可能在生物过程中发挥的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c832/3024258/94bc65a7f639/pcbi.1001051.g001.jpg

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