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首页> 外文期刊>Journal of chromatography, B. Analytical technologies in the biomedical and life sciences >Specific, sensitive and accurate liquid chromatographic-tandem mass spectrometric method for the measurement of ribavirin in rat and monkey plasma
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Specific, sensitive and accurate liquid chromatographic-tandem mass spectrometric method for the measurement of ribavirin in rat and monkey plasma

机译:用于测量大鼠和猴子血浆中利巴韦林测量的具体,灵敏和精确的液相色谱分谱法

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摘要

Ribavirin is a purine nucleoside analog with broad spectrum activity against a spectrum of DNA and RNA viruses. To facilitate pharmacokinetics studies, a LOC-MS-MS method for the analysis of ribavirin in rat and monkey plasma was developed and validated. The method involved the addition of acyclovir as an internal standard and protein precipitation with acetonitrile followed by separation by an Intertsil Silica column and quantification by a MS-MS equipped with a positive electrospray ionization in the multiple reaction monitoring mode. The MS-MS reaction was selected to monitor the 245→113 and 226→152 transitions for ribavirin and internal standard, respectively. The calibration curve was linear over a concentration range of 10-5000 ng/ml. The lower limit of quantitation was 10 ng/ml, the coefficient of variation (CV) was 8-11%, and the bias was 1-3%. Intra-day and inter-day analysis of QC samples at 30, 1500 and 3500 ng/ml indicate that the method was precise (CV<18%) and accurate (bias<13%). Ribavirin in rat and monkey plasma was stable at 5°C for at least 24 h, 0°C for at least 4 h, and after three freeze-thaw cycles. This specific, accurate and precise assay is useful in the study of the pharmacokinetics of this compound.
机译:利巴林是一种嘌呤核苷类似物,其具有广泛的DNA和RNA病毒的光谱活性。为了促进药代动力学研究,开发并验证了大鼠血浆中利巴韦林的LOC-MS-MS方法。该方法涉及添加Acyclovir作为内标和蛋白质沉淀,用乙腈,然后通过中间体硅胶柱分离,并通过在多反应监测模式下配备有正电喷雾电离的MS-MS进行定量。选择MS-MS反应以分别监测利巴韦林和内标的245→113和226→152转变。校准曲线在10-5000ng / ml的浓度范围内是线性的。定量下限为10ng / ml,变异系数(CV)为8-11%,偏差为1-3%。在30,1500和3500ng / mL时,QC样品的日期和白天分析表明该方法精确(CV <18%)和准确(偏见<13%)。 Ribavirin在大鼠和猴子血浆在5℃下稳定在5℃,至少24小时,0℃,至少4小时,以及三次冻融循环后。这种特异性,准确和精确的测定可用于研究该化合物的药代动力学。

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