Development and application of HPTLC method for estimation of Rivaroxaban and Aspirin in bulk drug and in-house tablet form

IF 1.8 Q3 CHEMISTRY, ANALYTICAL Journal of Chemical Metrology Pub Date : 2022-12-31 DOI:10.25135/jcm.78.2211.2636
Mehul M. Patel, Komal Bansal
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Abstract

: In the present work, simple, precise, accurate high-performance thin-layer chromatography was developed, optimized, and validated for quantitation of Rivaroxaban (RIV) and Aspirin (ASP). The developed method was applied for quantification of both the drugs simultaneously in bulk drug and in-house tablet formulation. In this study, the Camag Linomat V HPTLC system and win CATS software V1.4.7 were used. Both molecules were separated using a chromatographic method consisting of toluene: ethyl acetate: methanol: glacial acetic acid (6:3:0.5:0.5 v/v/v/v) as mobile phase and an aluminum pre-coated plate with silica gel 60 F254 as the stationary phase. Both drugs were detected at 256nm. With R f values of 0.23 and 0.72, respectively, Rivaroxaban and Aspirin were satisfactorily resolved. Moreover, as per the ICHQ2 (R1) guideline, Specificity, precision, accuracy, robustness, linearity, the limit of detection, and the limit of quantification were performed. The method was found linear in the range of 100-400 ng/band and 2000-8000 ng/band of Rivaroxaban and Aspirin, respectively. The precision of the method was determined by %RSD and it was found in range. In-house tablet formulation was prepared and applied the developed method for assay of RIV and ASP. The % Assay (%v/v) of RIV and ASP was found 100.61 %w/w and 100.29 %w/w. In a conclusion, the accurate, precise, sensitive, and robust HPTLC method was optimized, developed, and validated as per ICH Q2 (R1) guideline, which was applied for in-house tablet formulation. The result of the assay suggests that the developed method can be used for simultaneous estimation of RIV and ASP for their dosage form as a part of regulatory submission.
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hplc法测定利伐沙班和阿司匹林原料药和内服片剂含量的建立与应用
:在本工作中,开发、优化并验证了简单、精确、准确的高效薄层色谱法用于定量利伐沙班(RIV)和阿司匹林(ASP)。所开发的方法用于同时定量散装药物和内部片剂中的两种药物。本研究使用Camag Linomat V HPTLC系统和win CATS软件V1.4.7。使用由甲苯:乙酸乙酯:甲醇:冰醋酸(6:3:0.5:0.5v/v/v)作为流动相和用硅胶60F254作为固定相的铝预涂板组成的色谱法分离两种分子。两种药物均在256nm处检测到。在Rf值分别为0.23和0.72的情况下,利伐沙班和阿司匹林得到了令人满意的解决。此外,根据ICHQ2(R1)指南,进行了特异性、精密度、准确性、稳健性、线性、检测限和定量限。该方法在利伐沙班和阿司匹林的100-400纳克/带和2000-8000纳克/带范围内分别呈线性。方法的精密度用%RSD测定,在范围内。制备了自制片剂,并应用所开发的RIV和ASP测定方法。RIV和ASP的%含量测定(%v/v)分别为100.61%w/w和100.29%w/w。总之,根据ICH Q2(R1)指南对准确、准确、灵敏和稳健的HPTLC方法进行了优化、开发和验证,该指南适用于内部片剂配方。测定结果表明,作为监管提交的一部分,所开发的方法可用于同时估计RIV和ASP的剂型。
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来源期刊
Journal of Chemical Metrology
Journal of Chemical Metrology CHEMISTRY, ANALYTICAL-
CiteScore
2.30
自引率
15.40%
发文量
7
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