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Thermodynamic properties of duplex DNA containing a site-specific d(GpG) intrastrand crosslink formed by an antitumor dinuclear platinum complex

机译:双相的热力学性质 含有位点特异性d(GpG)链内交联的DNA形成 通过抗肿瘤的双核铂络合物

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摘要

Bifunctional polynuclear platinum compounds represent a novel class of metal-based antitumor drugs which are currently undergoing preclinical development. A typical agent is [{trans-PtCl(NH3)2}2H2N(CH2)4NH2]Cl2 (1,1/t,t), which coordinates to bases in DNA and forms various types of covalent crosslinks. It also forms a 1,2-d(GpG) intrastrand adduct, the equivalent of the major DNA lesion of ‘classical’ cisplatin. In the present study differential scanning calorimetry and spectroscopic techniques were employed to characterize the influence of this crosslink on the thermal stability and energetics of 20 bp DNA duplexes site-specifically modified by 1,1/t,t. Thermal denaturation data revealed that the crosslink of 1,1/t,t reduced thermal and thermodynamical stability of the duplex noticeably more than that of ‘classical’ cisplatin. The energetic consequences of the intrastrand crosslink at the d(GG) site are discussed in relation to the structural distortions induced by this adduct in DNA and to its recognition and binding by HMG domain proteins. It has been suggested that the results of the present work are consistent with different DNA binding modes of cisplatin and polynuclear bifunctional DNA-binding drugs, which might be relevant to their distinct biological effectiveness.
机译:双功能多核铂化合物代表了一类新型的基于金属的抗肿瘤药物,目前正在临床前开发中。典型的试剂是[{trans-PtCl(NH3)2} 2H2N(CH2)4NH2] Cl2(1,1 / t,t),其与DNA中的碱配位并形成各种类型的共价交联。它还形成了1,2-d(GpG)链内加合物,相当于“经典”顺铂的主要DNA损伤。在本研究中,采用差示扫描量热法和光谱技术表征了这种交联对位点特异性经1,1 / t,t修饰的20 bp DNA双链体的热稳定性和高能的影响。热变性数据显示,1,1 / t,t的交联降低了双链体的热稳定性和热力学稳定性,其稳定性明显优于“经典”顺铂。讨论了在d(GG)位点的链内交联的高能后果,涉及这种加合物在DNA中诱导的结构变形及其与HMG域蛋白的识别和结合。已经提出,本工作的结果与顺铂和多核双功能DNA结合药物的不同DNA结合模式一致,这可能与其独特的生物学功效有关。

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