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基于氧化还原的 DNA 堆积缺陷检测:来自杂交量子力学/分子力学分子动力学模拟的见解。

Redox-Based Defect Detection in Packed DNA: Insights from Hybrid Quantum Mechanical/Molecular Mechanics Molecular Dynamics Simulations.

机构信息

Laboratory of Computational Chemistry and Biochemistry, Institute of Chemical Sciences and Engineering, École Polytechnique Fédérale de Lausanne (EPFL), CH-1015 Lausanne, Switzerland.

出版信息

J Chem Theory Comput. 2023 Nov 28;19(22):8434-8445. doi: 10.1021/acs.jctc.3c01013. Epub 2023 Nov 14.

Abstract

The impact of an 8-oxoguanine (8oxoG) defect on the redox properties of DNA within the nucleosome core particle (NCP) was investigated employing hybrid quantum mechanical/molecular mechanics (QM/MM) molecular dynamics simulations of native and 8oxoG-containing NCP systems with an explicit representation of a biologically relevant environment. Two distinct NCP positions with varying solvent accessibility were considered for 8oxoG insertion. In both cases, it is found that the presence of 8oxoG drastically decreases the redox free energy of oxidation by roughly 1 eV, which is very similar to what was recently reported for free native and 8oxoG-containing DNA. In contrast, the effect of 8oxoG on the reorganization free energy is even smaller for packed DNA (decrease of 0.13 and 0.01 eV for defect-free and defect-containing systems, respectively) compared to the one for free DNA (0.25 eV), consistent with the increased rigidity of the NCP as compared to free DNA. Furthermore, the presence of an 8oxoG defect does not yield any significant changes in the packed DNA structure. Such a conclusion favors the idea that in the case of chromatin, defect-induced changes in DNA redox chemistry can also be exploited to detect damaged bases via DNA-mediated hole transfer.

摘要

研究了 8-氧鸟嘌呤(8oxoG)缺陷对核小体核心颗粒(NCP)中 DNA 的氧化还原性质的影响,方法是采用具有生物相关环境的显式表示的天然 NCP 系统和含 8oxoG 的 NCP 系统的混合量子力学/分子力学(QM/MM)分子动力学模拟。考虑了两种具有不同溶剂可及性的不同 NCP 位置来插入 8oxoG。在这两种情况下,都发现 8oxoG 的存在使氧化的自由能降低了约 1eV,这与最近报道的天然和含 8oxoG 的游离 DNA 非常相似。相比之下,与游离 DNA(0.25eV)相比,8oxoG 对包装 DNA 的重组自由能的影响更小(无缺陷和含缺陷系统分别降低了 0.13 和 0.01eV),这与 NCP 比游离 DNA 的刚性增加一致。此外,8oxoG 缺陷的存在不会导致包装 DNA 结构发生任何显著变化。这样的结论有利于这样一种观点,即在染色质的情况下,缺陷诱导的 DNA 氧化还原化学变化也可以通过 DNA 介导的空穴转移来检测受损碱基。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/05d7/10687876/9bf1639a7e38/ct3c01013_0001.jpg

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