Mantri Yogita, Lippard Stephen J, Baik Mu-Hyun
Department of Chemistry and School of Informatics, Indiana University, Bloomington, Indiana 47405, USA.
J Am Chem Soc. 2007 Apr 25;129(16):5023-30. doi: 10.1021/ja067631z. Epub 2007 Apr 3.
The bifunctional binding of the anticancer drug cisplatin to two adjacent nucleobases in DNA is modeled using density functional theory. Previous experimental studies revealed that cisplatin binding to adjacent guanine and adenine is sensitive to nucleobase sequence. Whereas AG 1,2-intrastrand cross-links are commonly observed, the analogous GA adducts are not known. This study focuses on understanding this directional preference by constructing a full reaction profile using quantum chemical simulation methods. Monofunctional and bifunctional cisplatin adducts were generated, and the transition states that connect them were located for the dinucleotides d(pApG) and d(pGpA), assuming that initial platination takes place at the guanine site. Our computer simulations reveal a significant kinetic preference for formation of the AG over the GA adduct. The activation free energies of approximately 23 kcal/mol for AG and approximately 32 kcal/mol for GA suggest that bifunctional closure is approximately 6 orders of magnitude faster for AG than for GA. A strong hydrogen bond between one of the ammine ligands of cisplatin and the 5' phosphate group of the DNA backbone is responsible for the stabilization of the transition state that affords the AG adduct. This interaction is absent in the transition state that leads to the GA adduct because the right-handed helix of the DNA backbone places the phosphate out of reach for the ammine ligand. We found only an insignificant thermodynamic difference between AG and GA adducts and conclude that the preference of AG over GA binding is largely under kinetic control. The puckering of the deoxyribose ring plays an important role in determining the energetics of the bifunctional platination products. Whereas the 3'-nucleoside remains in the native C2'-endo/C3'-exo form of B-DNA, the deoxyribose of the 5'-nucleoside always adopts the C2'-exo/C3'-endo puckering in our simulations. A detailed analysis of the energies and structures of the bifunctional adducts revealed that the observed sugar puckering patterns are necessary for platinum to bind in a relaxed coordination geometry.
利用密度泛函理论对抗癌药物顺铂与DNA中两个相邻核碱基的双功能结合进行了建模。先前的实验研究表明,顺铂与相邻鸟嘌呤和腺嘌呤的结合对核碱基序列敏感。虽然AG 1,2-链内交联很常见,但类似的GA加合物尚不清楚。本研究通过使用量子化学模拟方法构建完整的反应剖面图来理解这种方向偏好。生成了单功能和双功能顺铂加合物,并确定了连接它们的过渡态,用于二核苷酸d(pApG)和d(pGpA),假设初始铂化发生在鸟嘌呤位点。我们的计算机模拟揭示了形成AG加合物相对于GA加合物有显著的动力学偏好。AG的活化自由能约为23 kcal/mol,GA的活化自由能约为32 kcal/mol,这表明双功能闭合对于AG比对GA快约6个数量级。顺铂的一个氨配体与DNA主链的5'磷酸基团之间的强氢键负责稳定提供AG加合物的过渡态。在导致GA加合物的过渡态中不存在这种相互作用,因为DNA主链的右手螺旋使磷酸基团超出了氨配体的作用范围。我们发现AG和GA加合物之间只有微不足道的热力学差异,并得出结论,AG比对GA结合的偏好主要受动力学控制。脱氧核糖环的褶皱在决定双功能铂化产物的能量方面起着重要作用。在我们的模拟中,虽然3'-核苷保持在B-DNA的天然C2'-内/ C3'-外形式,但5'-核苷的脱氧核糖总是采用C2'-外/ C3'-内褶皱。对双功能加合物的能量和结构的详细分析表明,观察到的糖褶皱模式对于铂以松弛的配位几何结构结合是必要的。