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抗血小板药物噻氯匹定与小牛胸腺 DNA 相互作用的分子光谱和热力学研究。

Molecular spectroscopic and thermodynamic studies on the interaction of anti-platelet drug ticlopidine with calf thymus DNA.

机构信息

Department of Biochemistry, Faculty of Life Sciences, A.M. University, Aligarh, UP 202002, India.

Steroid Research Laboratory, Department of Chemistry, Aligarh Muslim University, Aligarh 202002, India.

出版信息

Spectrochim Acta A Mol Biomol Spectrosc. 2017 Nov 5;186:66-75. doi: 10.1016/j.saa.2017.05.073. Epub 2017 Jun 12.

DOI:10.1016/j.saa.2017.05.073
PMID:28614751
Abstract

Ticlopidine is an anti-platelet drug which belongs to the thienopyridine structural family and exerts its effect by functioning as an ADP receptor inhibitor. Ticlopidine inhibits the expression of TarO gene in S. aureus and may provide protection against MRSA. Groove binding agents are known to disrupt the transcription factor DNA complex and consequently inhibit gene expression. Understanding the mechanism of interaction of ticlopidine with DNA can prove useful in the development of a rational drug designing system. At present, there is no such study on the interaction of anti-platelet drugs with nucleic acids. A series of biophysical experiments were performed to ascertain the binding mode between ticlopidine and calf thymus DNA. UV-visible and fluorescence spectroscopic experiments confirmed the formation of a complex between ticlopidine and calf thymus DNA. Moreover, the values of binding constant were found to be in the range of 10M, which is indicative of groove binding between ticlopidine and calf thymus DNA. These results were further confirmed by studying the effect of denaturation on double stranded DNA, iodide quenching, viscometric studies, thermal melting profile as well as CD spectral analysis. The thermodynamic profile of the interaction was also determined using isothermal titration calorimetric studies. The reaction was found to be endothermic and the parameters obtained were found to be consistent with those of known groove binders. In silico molecular docking studies further corroborated well with the experimental results.

摘要

噻氯匹定是一种抗血小板药物,属于噻吩并吡啶结构家族,通过作为 ADP 受体抑制剂发挥作用。噻氯匹定抑制金黄色葡萄球菌 TarO 基因的表达,可能对耐甲氧西林金黄色葡萄球菌(MRSA)提供保护。沟槽结合剂已知会破坏转录因子 DNA 复合物,从而抑制基因表达。了解噻氯匹定与 DNA 的相互作用机制可能有助于开发合理的药物设计系统。目前,尚无关于抗血小板药物与核酸相互作用的此类研究。进行了一系列生物物理实验以确定噻氯匹定与小牛胸腺 DNA 之间的结合模式。紫外可见和荧光光谱实验证实了噻氯匹定与小牛胸腺 DNA 之间形成了复合物。此外,结合常数的值被发现处于 10M 的范围内,这表明噻氯匹定与小牛胸腺 DNA 之间存在沟槽结合。通过研究变性对双链 DNA 的影响、碘猝灭、粘度研究、热融解曲线以及 CD 光谱分析进一步证实了这些结果。还使用等温滴定量热法研究确定了相互作用的热力学特性。反应是吸热的,获得的参数与已知的沟槽结合剂的参数一致。计算机分子对接研究进一步与实验结果相符。

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