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DNA 链间交联的热稳定性。

Thermal stability of DNA with interstrand crosslinks.

机构信息

Department of Physics, National Central University, Chungli 32001, Taiwan.

出版信息

Biopolymers. 2012 Oct;97(10):807-17. doi: 10.1002/bip.22077.

Abstract

Although many anticancer drugs exert their biological activity by forming DNA interstrand crosslinks (ICLs), the thermodynamics of biologically relevant long crosslinked DNAs has not been intensively studied in contrast to short duplexes. Here, we carry out computer modeling of the shift of melting temperature of long DNAs caused by ICLs taking into account crosslinking effect in itself and concomitant local alterations in the free energy (δG) of the helix-coil transition at sites of ICLs. Depending on δG, DNA interstrand crosslinks at per nucleotide concentration r = 0.05 can change the melting temperature by value from -17 to +47°C, and the influence weakly depends on DNA sequence and GC content. A change in melting temperature caused by introduction of interstrand crosslinking in modified DNA at sites of modifications also depends on δG and varies from 0 to +12°C. Comparison with experiment for the three platinum crosslinking compounds demonstrates utility of the theoretical method for understanding how crosslinking compounds can influence the melting behavior. On the basis of the method, interdependence of local distortions and crosslinking in itself was studied for thermal effect of ICLs. A method for evaluating the nature of the structural alteration that produces a change in thermal stability for short crosslinked DNA is also proposed. The methods can be used for comparative thermodynamic characterization of various DNA crosslinking agents.

摘要

尽管许多抗癌药物通过形成 DNA 链间交联(ICLs)发挥其生物活性,但与短双链体相比,生物相关的长交联 DNA 的热力学尚未得到深入研究。在这里,我们进行了计算机建模,研究了 ICLs 引起的长 DNA 熔点变化,同时考虑了交联本身的影响以及 ICL 位置处螺旋-线圈转变的自由能(δG)的伴随局部变化。根据 δG,每核苷酸浓度 r = 0.05 的 DNA 链间交联可以使熔点发生从-17°C 到+47°C 的变化,并且这种影响与 DNA 序列和 GC 含量的关系较弱。在修饰的 DNA 中引入交联在修饰部位也会引起熔点的变化,这取决于 δG,并且变化范围从 0°C 到+12°C。与三种铂交联化合物的实验比较表明,该理论方法对于理解交联化合物如何影响熔点行为非常有用。在此基础上,研究了局部扭曲和交联本身之间的相互依赖性,以研究 ICLs 的热效应。还提出了一种用于评估产生短交联 DNA 热稳定性变化的结构改变性质的方法。这些方法可用于各种 DNA 交联剂的比较热力学表征。

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