经验证的稳定性指示反相高效液相色谱法测定Daclatasvir片中的含量。

IF 1.8 Q3 PHARMACOLOGY & PHARMACY Turkish Journal of Pharmaceutical Sciences Pub Date : 2023-08-22 DOI:10.4274/tjps.galenos.2022.87393
Hemlata M Nimje, Smita J Pawar, Meenakshi N Deodhar
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引用次数: 1

摘要

目的:建立一种精确、灵敏、有效的反相高效液相色谱(RP-HPLC)方法来评估直接作用抗病毒药物daclatasvir (DCV),并评估DCV在药物和片剂制剂中的稳定性。目前的研究是在不同的应激条件下显示稳定性,包括水解(酸性、碱性和中性)、氧化和光解。材料和方法:所有实验均在Agilent 1100高效液相色谱仪上进行,柱柱为不锈钢Hypersil C18,粒径为5 μm,尺寸为4.6 x 250 mm。流动相为乙腈:0.05% o-磷酸(50:50 v/v),流速0.7 mL/min,检测波长315 nm。结果:该方法的线性和范围、准确度、精密度、检出限、定量限和鲁棒性符合国际统一委员会(ICH)的要求。结果令人满意。在酸性条件下,DCV降解产物的停留时间(tR)分别为3.863、4.121和4.783 min,串联质谱(MS/MS)扫描结果为m/z 339.1、561.2个片段离子。在基本条件下,DCV降解物的tR值分别为5.188、5.469 min, MS/MS扫描的m/z值分别为294.1、339.1、505.2、527.2个碎片离子。在氧化条件下,DCV降解产物的tR值为4.038 min, MS/MS扫描结果显示m/z为301.1和339.1。结论:在不同的应力条件下,所有的质量碎片都表现出额外的降解。这将有助于确定降解物的结构及其途径。在中性和光解条件下未观察到降解。
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Validated Stability-Indicating RP-HPLC Method for Daclatasvir in Tablets.

Objectives: The current study goal was to create a precise, sensitive, and validated reverse phase-high performance liquid chromatography (RP-HPLC) method for assessing the direct-acting antiviral daclatasvir (DCV) as well as to evaluate the stability of DCV in both drug and tablet formulations. The current investigation was to display stability indicating methods under different stress conditions, including hydrolysis (acidic, basic, and neutral), oxidation, and photolysis.

Materials and methods: All experiments were performed on HPLC Agilent 1100 with a stainless steel Hypersil C18 column having a particle size of 5 μm and a dimension of 4.6 x 250 mm. The mobile phase chosen was acetonitrile: 0.05% o-phosphoric acid (50:50 v/v) in isocratic mode with 0.7 mL/min flow rate and wavelength 315 nm was selected for detection.

Results: This method was validated for linearity and range, accuracy, precision, limit of detection, limit of quantification, and robustness in accordance with International Council for Harmonisation (ICH) requirements. The results were satisfactory. It was observed that retention time (tR) was 3.760 ± 0.01 min. In acidic conditions, DCV degradans show tR at 3.863, 4.121, and 4.783 min and tandem mass spectrometry (MS/MS) spectra scans had m/z 339.1, 561.2 fragment ions. In basic condition, DCV degradans show tR at 5.188, 5.469 min and MS/MS spectra scans having m/z 294.1, 339.1, 505.2, 527.2 fragment ions. In oxidation conditions, DCV degradans shows tR at 4.038 min and MS/MS spectra scans having m/z 301.1 and 339.1 fragment ions were observed.

Conclusion: All the mass fragments exhibited additional degradation observed for different stress conditions. This will help to identify the structure of the degradant and its pathways. No degradation was observed in neutral and photolytic conditions.

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