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Spectroscopic and Molecular Docking Investigations on the Effect of the Interaction Between Cefoperazone Sodium and Papain to Drug Efficacy

机译:光谱和分子对接调查之间的相互作用的影响头孢哌酮钠和木瓜蛋白酶药物功效

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Under the experimental condition of pH=7.40, papain (PAPA) was used as the detection object, and the binding behavior of cefoperazone sodium (CFZ) and PAPA at three temperatures was studied by multi-spectroscopy and molecular docking. The results showed that CFZ can effectively quench the endogenous fluorescence of PAPA, form a 1:1 complex, and change the conformation of PAPA. At 293 K, the fluorescence intensity of the system had a good linear relationship with the CFZ concentration in the range of 4.0×10~(-6) ~ 1.0×10-4 mol/L. The detection limit of the method was 2.43×10-6 mol/L (n=10), indicating that the reaction can be used to achieve rapid determination of CFZ content in the actual drug. Based on the experimental data, a mathematical model combining CFZ and PAPA was established. When the peak plasma concentration of CFZ was 106.0 mg/L after intravenous infusion of 1 g, the drug binding rate of CFZ-PAPA system was 2.70 %, indicating the combination of CFZ and PAPA did not affect the efficacy of CFZ, that is, when taking CFZ, it is safe to consume PAPA. Molecular simulation studies had showed that the interaction between CFZ and PAPA had not only electrostatic forces but also hydrogen bonding, which was consistent with the results of spectroscopy and thermodynamic studies.
机译:的实验条件下pH = 7.40,木瓜蛋白酶(爸爸)作为检测对象,和头孢哌酮钠的具有约束力的行为(CFZ)和爸爸在三个温度进行了研究multi-spectroscopy和分子对接。结果表明,CFZ可以有效地熄灭爸爸的内源荧光,形成1:1复杂的,爸爸的构象变化。293 K,系统的荧光强度CFZ有很好的线性关系浓度范围为4.0×10 ~ (6)~1.0 mol / L 4×打败。为2.43×10 - 6 mol / L (n = 10),表明可以用来实现快速反应CFZ含量测定实际的药物。基于实验数据,一个数学模型结合CFZ和爸爸成立。当CFZ的血浆浓度峰值106.0 mg / L, 1 g的静脉输液,CFZ-PAPA系统的药物结合率为2.70%,指示CFZ和爸爸做的不影响CFZ的功效,当CFZ,爸爸是安全消费。仿真研究表明,CFZ和爸爸之间的互动不仅静电力还有氢键,这是一致的结果吗光谱和热力学研究。

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