Bioanalytical Method Development and Validation for Determination of Rifampicin and Quercetin in Rat Plasma by UHPLC-MS/MS: Applications to Pharmacokinetic Study

Devangkumar Tandel, K. Patel, V. Thakkar, A. Sakure, T. Gandhi
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引用次数: 1

Abstract

Abstract UHPLC-MS/MS was utilised to quantitatively analyse Rifampicin and Quercetin-loaded Liquisolid compact in rat plasma. The UPLC Acquity C18 (1.7 μm, 2.1 × 15 mm) column and 0.5 ml/min were used to separate the analyte. In a low-pressure gradient mode, A: In water 0.1 % formic acid and B: In acetonitrile 0.1 % formic acid as the mobile phase. Sample pre-treatment was performed by protein precipitation technique with methanol and acetonitrile (1:1) from rat plasma. As an internal standard (IS), the analyte was found by tracking precursor-to-product ion transformations of 823 → 791.3 m/z for rifampicin, 303 → 257 m/z for quercetin, and 138 → 121 m/z for isoniazid in MRM mode. The proposed technique was validated for precisions (Intraday and Interday) accuracy, linearity, quantification at lower limits, and analyte recovery. The findings showed that the plasma samples inter and intra-day precision and consistency values were determined to be within the acceptable range. After orally administering Liquid solid compact and pure drug solution, which showed a substantial difference in the pace and extent of absorption, the method’s suitability for determining the pharmacokinetic profile of each drug was tested. GRAPHICAL ABSTRACT
UHPLC-MS/MS法测定大鼠血浆中利福平和槲皮素的生物分析方法的建立与验证:在药动学研究中的应用
摘要采用高效液相色谱-质谱联用技术对大鼠血浆中含有利福平和槲皮素的液质致密物进行定量分析。色谱柱为UPLC Acquity C18 (1.7 μm, 2.1 × 15 mm),分离速度为0.5 ml/min。在低压梯度模式下,a:以0.1%甲酸为水,B:以0.1%甲酸为乙腈的流动相。样品前处理采用大鼠血浆甲醇与乙腈(1:1)蛋白沉淀技术。作为内标物(IS),在MRM模式下,通过跟踪前体到产物的离子转换,发现利福平为823→791.3 m/z,槲皮素为303→257 m/z,异烟肼为138→121 m/z。该方法的精密度(intrday和Interday)、准确度、线性度、下限定量和分析物回收率均得到验证。结果表明,血浆样品的日间和日间精密度和一致性值均在可接受范围内。口服液体、固体致密药溶液和纯药溶液,在吸收速度和吸收程度上有很大差异,并对该方法测定每种药物的药代动力学谱的适用性进行了测试。图形抽象
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CiteScore
2.30
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