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顺铂链内交联对一段20聚体DNA双链体的构象、热稳定性及能量学的影响

Influence of cisplatin intrastrand crosslinking on the conformation, thermal stability, and energetics of a 20-mer DNA duplex.

作者信息

Poklar N, Pilch D S, Lippard S J, Redding E A, Dunham S U, Breslauer K J

机构信息

Department of Chemistry, Rutgers-The State University of New Jersey, New Brunswick 08903, USA.

出版信息

Proc Natl Acad Sci U S A. 1996 Jul 23;93(15):7606-11. doi: 10.1073/pnas.93.15.7606.

Abstract

cis-Diamminedichloroplatinum(II) (cisplatin) is a widely used anticancer drug that binds to and crosslinks DNA. The major DNA adduct of the drug results from coordination of two adjacent guanine bases to platinum to form the intrastrand crosslink cis-[Pt(NH3)2[d(GpG)-N7(1), -N7(2)]] (cis-Pt-GG). In the present study, spectroscopic and calorimetric techniques were employed to characterize the influence of this crosslink on the conformation, thermal stability, and energetics of a site-specifically platinated 20-mer DNA duplex. CD spectroscopic and thermal denaturation data revealed that the crosslink alters the structure of the host duplex, consistent with a shift from a B-like to an A-like conformation; lowers its thermal stability by approximately 9 degrees C; and reduces its thermodynamic stability by 6.3 kcal/mol at 25 degrees C, most of which is enthalpic in origin; but it does not alter the two-state melting behavior exhibited by the parent, unmodified duplex, despite the significant crosslink-induced changes noted above. The energetic consequences of the cis-Pt-GG crosslink are discussed in relation to the structural perturbations it induces in DNA and to how these crosslink-induced perturbations might modulate protein binding.

摘要

顺二氯二氨合铂(II)(顺铂)是一种广泛使用的抗癌药物,它能与DNA结合并使其交联。该药物的主要DNA加合物是由两个相邻的鸟嘌呤碱基与铂配位形成链内交联顺式-[Pt(NH3)2[d(GpG)-N7(1), -N7(2)]](顺铂-GG)产生的。在本研究中,采用光谱和量热技术来表征这种交联对位点特异性铂化的20聚体DNA双链体的构象、热稳定性和能量学的影响。圆二色光谱和热变性数据表明,这种交联改变了宿主双链体的结构,这与从B型构象向A型构象的转变一致;使其热稳定性降低了约9摄氏度;在25摄氏度时,其热力学稳定性降低了6.3千卡/摩尔,其中大部分是由焓引起的;尽管有上述交联引起的显著变化,但它并没有改变未修饰的亲本双链体所表现出的两态熔解行为。本文讨论了顺铂-GG交联的能量后果,涉及它在DNA中引起的结构扰动以及这些交联引起的扰动如何调节蛋白质结合。

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