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首页> 外文期刊>Biophysical Journal >A statistical thermodynamic model for investigating the stability of DNA sequences from oligonucleotides to genomes
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A statistical thermodynamic model for investigating the stability of DNA sequences from oligonucleotides to genomes

机译:统计热力学模型,用于研究从寡核苷酸到基因组的DNA序列的稳定性

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摘要

We describe the development and testing of a simple statistical mechanics methodology for duplex DNA applicable to sequences of any composition and extensible to genomes. The microstates of a DNA sequence are modeled in terms of blocks of basepairs that are assumed to be fully closed (paired) or open. This approach generates an ensemble of bubblelike microstates that are used to calculate the corresponding partition function. The energies of the microstates are calculated as additive contributions from hydrogen bonding, basepair stacking, and solvation terms parameterized from a comprehensive series of molecular dynamics simulations including solvent and ions. Thermodynamic properties and nucleotide stability constants for DNA sequences follow directly from the partition function. The methodology was tested by comparing computed free energies per basepair with the experimental melting temperatures of 60 oligonucleotides, yielding a correlation coefficient of -0.96. The thermodynamic stability of genicongenic regions was tested in terms of nucleotide stability constants versus sequence for the Escherichia coli K-12 genome. It showed clear differentiation of the genes from promoters and captures genic regions with a sensitivity of 0.94. The statistical thermodynamic model presented here provides a seemingly new handle on the challenging problem of interpreting genomic sequences.
机译:我们描述了一种简单的统计力学方法论的发展和测试,该方法适用于可应用于任何成分且可扩展至基因组的双链体DNA。 DNA序列的微状态是根据碱基对的块进行建模的,这些碱基对的块被假定为完全封闭(配对)或开放。这种方法生成了一组气泡状微状态,用于计算相应的分区函数。微状态的能量计算为氢键,碱基对堆积和溶剂化项的累加贡献,而溶剂化项是通过一系列全面的分子动力学模拟(包括溶剂和离子)进行参数化的。 DNA序列的热力学性质和核苷酸稳定常数直接来自分配函数。通过将每个碱基对的计算出的自由能与60个寡核苷酸的实验解链温度进行比较来测试该方法,得出相关系数为-0.96。就大肠杆菌K-12基因组的核苷酸稳定性常数对序列而言,测试了基因/非基因区的热力学稳定性。它显示了基因与启动子的明显区别,并以0.94的灵敏度捕获了基因区域。本文介绍的统计热力学模型为解释基因组序列这一具有挑战性的问题提供了看似新的方法。

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