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Determination of paracetamol in pure and pharmaceutical dosage forms by pulse perturbation technique.

机译:通过脉冲微扰技术测定纯净和药物剂型中的扑热息痛。

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摘要

A new procedure for kinetic determination of paracetamol in pharmaceuticals is proposed. The method is based on potentiometric monitoring of the concentration perturbations of the matrix reaction system being in a stable non-equilibrium stationary state close to the bifurcation point. In the case considered as the matrix system, the Bray-Liebhafsky oscillatory reaction is used. The response of the matrix system to the perturbations by different concentrations of paracetamol is followed by a Pt-electrode. Proposed method relies on the linear relationship between maximal potential shift, DeltaEm, and the logarithm of added paracetamol amounts. It is obtained in optimized experimental conditions for variable amounts of paracetamol in the range 0.0085 and 1.5 micromol. The sensitivity and precision of proposed method were quite good (0.0027 micromol as the limit of detection and 2.4% as R.S.D.). Some aspects of possible chemical interactions between paracetamol and matrix are discussed. Applicability of the proposed method to the direct determination of paracetamol in pharmaceutical formulations was demonstrated.
机译:提出了一种动力学测定药物中扑热息痛的新方法。该方法基于电位计监测基质反应体系在接近分叉点的稳定非平衡稳态下的浓度扰动。在考虑为矩阵系统的情况下,使用Bray-Liebhafsky振荡反应。基质系统对不同浓度的扑热息痛对微扰的响应后是Pt电极。提出的方法依赖于最大电势位移,DeltaEm和对乙酰氨基酚添加量的对数之间的线性关系。它是在优化实验条件下,对乙酰氨基酚的量在0.0085至1.5 micromol范围内变化而获得的。所提方法的灵敏度和精密度都很好(检测限为0.0027微摩尔,R.S.D。为2.4%)。讨论了扑热息痛与基质之间可能的化学相互作用的一些方面。证明了该方法可直接测定药物制剂中对乙酰氨基酚的适用性。

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