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Spectroscopic Methods for Quantifying Gabapentin: Framing the Methods without Derivatization and Application to Different Pharmaceutical Formulations

机译:用于量化加巴亨坦的光谱方法:构成不衍生化的方法和应用于不同的药物制剂

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摘要

This work aimed at analyzing the performance of direct spectroscopic methods for the quantification of gabapentin (GABAp), given the lack of previous studies, in comparison with the more reviewed and complex derivatization techniques, discussing their susceptibility to the pharmaceutical formulations. All of the methods analyzed showed high selectivity for this pharmaceutical analyte, with recoveries close to 100%. Absorption spectroscopy without derivatization yielded better sensitivity and lower limits of detection and quantification of gabapentin in aqueous solution (AqSol method) when compared with other solvents, such as acidic solution or ethanol/water mixture. Derivatization with sodium hypochlorite presented the highest precision, whereas derivatization with vanillin exhibited the highest accuracy. The best method for GABAp quantification in terms of highest sensitivity, lowest limits of detection, and quantification, and also with good precision and accuracy, proved to be fluorescence with derivatization by 4-chloro-7-nitrobenzofurazan. The effect of the pharmaceutical formulation (nature of excipients) was tested for the most robust and sensitive methods, with and without derivatization, on capsules of five commercial brands. Recoveries in the range of 97.9-101.5% proved that there are no matrix interfering effects. Although not presenting the best performance in all the parameters evaluated, the AqSol method, due to its simplicity, proved to be suitable for the quantification of GABAp in capsules and tables containing the molecule as the active ingredient.
机译:鉴于缺乏先前研究的缺乏先前研究,鉴于缺乏先前的研究,旨在分析鉴于缺乏先前的研究,旨在进行分析的这种作品。分析的所有方法显示出该药物分析物的高选择性,恢复接近100%。与其他溶剂相比,没有衍生化的吸收光谱法产生更好的敏感性和水溶液(AQSOL方法)中的甘地蛋白的检测和定量较低限制。用次氯酸钠衍生化呈现最高精度,而用香草蛋白的衍生化表现出最高的精度。在最高敏感性,最低检测限率和定量方面,以及良好的精度和精度的最佳方法,并被证明是4-氯-7-硝基苯脲尿嘧啶的荧光。药物制剂(赋形剂的性质)的效果用于最强大,敏感的方法,在五个商业品牌的胶囊上有和不衍生化。 97.9-101.5%的回收证明,没有矩阵干扰效应。虽然没有在评估的所有参数中呈现最佳性能,但由于其简单性而被证明的AQSOL方法被证明适用于胶囊中的胶囊和包含分子作为活性成分的表格的量化。

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