Schmitz H U, Hübner W
Institut für Physikalische Chemie, Universität Freiburg, Germany.
Biophys Chem. 1993 Nov;48(1):61-74. doi: 10.1016/0301-4622(93)80042-h.
The complete thermodynamic profile for the non-intercalative binding of berenil to the alternating copolymer poly d(AT) and to the homopolymer poly (dA) x poly (dT) was investigated. Differential Scanning Calorimetry (DSC) and UV absorbance spectroscopy have been used to characterize and to compare the binding of berenil to the different synthetic polymers. Both double stranded DNA's show two types of binding; one stronger binding mode at low berenil concentrations and a weaker, in the case of poly d(AT)-berenil complexes slightly cooperative binding mode at higher drug to base pair ratios. For the interaction of berenil with poly d(AT) the thermodynamic data delta G(bind)0 = -33 kJ/mol drug, delta H(bind)0 = -29 kJ/mol of drug and delta S(bind)0 = +13 J/Kmol of drug were calculated. For the minor groove binding of berenil to poly (dA) x poly (dT) the following values were obtained: delta G(bind)0 = -34 kJ/mol of drug, delta H(bind)0 = -25 kJ/mol of drug and delta S(bind)0 = +30 J/Kmol of drug. Temperature-dependent UV absorbance spectroscopy revealed for both duplexes a biphasic "melting" behavior. However, the saturated nucleic acids (drug to base pair ratio 0.33) "melted" monophasically and with a decreased length of the cooperative unit. The obtained apparent equilibrium constants K(app) for the complexation with the discharged drug molecule showed to be a sensitive function of the ionic environment. But in contradiction to the expected release of two counterions into the solvent only a value of 1.0 was observed for the alternating copolymer poly d(AT). The complexation of berenil with poly (dA) x poly (dT) is followed by a release of 1.4 ions indicating stronger electrostatic interactions. For both polynucleotides the predicted release of two ions is not achieved. This is due to the presence of a binding mode, which involves less electrostatic interactions. From the complete data set it is proposed that the mode of binding is closely related to that found for the analogue minor groove binders DAPI and netropsin.
研究了贝尼尔与交替共聚物聚d(AT)和均聚物聚(dA)×聚(dT)的非嵌入结合的完整热力学曲线。差示扫描量热法(DSC)和紫外吸收光谱法已被用于表征和比较贝尼尔与不同合成聚合物的结合。两种双链DNA都表现出两种结合类型;一种是在低贝尼尔浓度下更强的结合模式,另一种是较弱的结合模式,在聚d(AT)-贝尼尔复合物中,在较高的药物与碱基对比例下,结合模式略有协同。对于贝尼尔与聚d(AT)的相互作用,计算出热力学数据ΔG(bind)0 = -33 kJ/mol药物,ΔH(bind)0 = -29 kJ/mol药物,ΔS(bind)0 = +13 J/Kmol药物。对于贝尼尔与聚(dA)×聚(dT)的小沟结合,得到以下值:ΔG(bind)0 = -34 kJ/mol药物,ΔH(bind)0 = -25 kJ/mol药物,ΔS(bind)0 = +30 J/Kmol药物。温度依赖性紫外吸收光谱显示两种双链体都有双相“熔解”行为。然而,饱和核酸(药物与碱基对比例为0.33)“单熔解”,且协同单元长度减小。与释放的药物分子络合得到的表观平衡常数K(app)显示是离子环境的敏感函数。但与预期的两个抗衡离子释放到溶剂中相反,交替共聚物聚d(AT)仅观察到值为1.0。贝尼尔与聚(dA)×聚(dT)的络合伴随着1.4个离子的释放,表明静电相互作用更强。对于两种多核苷酸,都没有实现预测的两个离子的释放。这是由于存在一种涉及较少静电相互作用的结合模式。根据完整的数据集,提出结合模式与类似物小沟结合剂DAPI和纺锤菌素的结合模式密切相关。
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