亲水作用液相色谱法同时分析抗病毒药物剂型的ZIC-HILIC色谱柱比较

IF 0.7 4区 医学 Q4 PHARMACOLOGY & PHARMACY Current Pharmaceutical Analysis Pub Date : 2023-10-01 DOI:10.2174/0115734129252205230920052737
Sohair Salah Ahmed, Ashraf Rasheed
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引用次数: 0

摘要

背景:抗病毒药物至关重要,因为许多病毒可产生致命感染,正如我们最近在COVID-19大流行中看到的那样。抗病毒药物可以在病毒生命周期的多个阶段对抗病毒,包括神经氨酸酶、核酸合成、蛋白酶和病毒粒子融合或进入[1]。目的:抗病毒药物在反相液相色谱中保留率差,这使得使用高效液相色谱分析抗病毒药物混合物变得困难。利用两性离子亲水性相互作用液相色谱(ZICHILIC),重点研究了三种抗病毒药物在药物制剂中作为有效成分的同时定量。此外,还讨论了两个固定相中两个电荷之间的间隔长度对抗病毒药物保留行为的影响。方法:采用自制的两种固定相(ZIC1-HILIC和ZIC5-HILIC)对3种抗病毒药物进行定性和定量分析,以紫外为检测器。考察了有机改性剂浓度、缓冲液浓度和pH值等色谱条件。结果:优化参数后,所设计的方法可用于3种抗病毒药物的定量分析。初步结果表明,目前分离和确定这三种抗病毒药物的方法是敏感、稳健和有效的。结果表明,该方法重复性好,线性范围宽(0.1 ~ 16.5 μgml-1),灵敏度高(LOD 0.04 ~ 0.072 μgml-1)。该方法的RSD值小于1。结论:两种ZIC-HILIC固定相的抗病毒药物以亲水性和离子交换相互作用混合模式为主。与链长较短的ZIC1-HILIC固定相相比,ZIC5-HILIC固定相对三种抗病毒药物的检测和定量限较低,保留时间较长。
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Comparison of ZIC-HILIC Columns for the Simultaneous Analysis of Antiviral Drugs in Dosage Forms by Hydrophilic Interaction Liquid Chromatography
Background:: Antiviral drugs are vital since many viruses can produce fatal infections, as we have recently seen with the COVID-19 pandemic. Antiviral drugs can battle viruses at multiple stages of their life cycles, including neuraminidase, nucleic acid synthesis, protease, and virion fusion or entry [1]. Objective:: Antiviral drugs have poor retention in reversed-phase liquid chromatography, which makes it difficult to analyze a mixture of antiviral medications using high-performance liquid chromatography. Using zwitterionic hydrophilic interaction liquid chromatography (ZICHILIC), the paper highlights the simultaneous quantification of three antiviral drugs as active constituents in pharmaceutical formulations. Moreover, the influence of the length of the spacer between the two charges in two stationary phases on the retention behavior of antiviral drugs has been discussed. Methods:: Two homemade stationary phases (ZIC1-HILIC and ZIC5-HILIC) were utilized for the qualitative and quantitative analysis of three antiviral drugs, and UV was used as the detector. Several chromatographic conditions were examined, such as the organic modifier concentration, buffer concentration, and pH value. Results:: After optimizing the parameters, the devised method was applied to analyse three antiviral medications quantitatively. The initial results demonstrated the current procedure for separating and determining these three antiviral drugs to be sensitive, robust, and effective. Consequently, the present method has shown excellent repeatability, a broad linear range (0.1- 16.5 μgml-1), and excellent sensitivity (LOD 0.04-0.072 μgml-1). The RSD value of the method was less than 1. Conclusion:: A mixed mode of hydrophilic and ion exchange interactions was the predominant mode of antiviral medications with two ZIC-HILIC stationary phases. The ZIC5-HILIC stationary phase had a lower detection and limit of quantitation for three antiviral drugs and a prolonged retention time compared to the ZIC1-HILIC stationary phase with a shorter chain length.
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来源期刊
CiteScore
1.50
自引率
0.00%
发文量
85
审稿时长
3 months
期刊介绍: Aims & Scope Current Pharmaceutical Analysis publishes expert reviews and original research articles on all the most recent advances in pharmaceutical and biomedical analysis. All aspects of the field are represented including drug analysis, analytical methodology and instrumentation. The journal is essential to all involved in pharmaceutical, biochemical and clinical analysis.
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