UPLC-MS/MS测定大鼠舌下静脉注射阿西替尼的血药浓度及其药动学研究

冯炎林; 洪滟; 田伟强

引用本文:	冯炎林,洪滟,田伟强.UPLC-MS/MS测定大鼠舌下静脉注射阿西替尼的血药浓度及其药动学研究[J].中国现代应用药学,2017,34(9):1304-1308.
	FENG Yanlin,HONG Yan,TIAN Weiqiang.Study on Plasma Concentration and Pharmacokinetics of Axitinib After Intravenous Administration in Rats by UPLC-MS/MS[J].Chin J Mod Appl Pharm(中国现代应用药学),2017,34(9):1304-1308.

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UPLC-MS/MS测定大鼠舌下静脉注射阿西替尼的血药浓度及其药动学研究
冯炎林, 洪滟, 田伟强
温州医科大学附属五院丽水市中心医院药学部, 浙江丽水 323000

摘要:

目的建立UPLC-MS/MS对舌下静脉注射大鼠血浆中阿西替血药浓度的检测方法，并进行其药动学研究。方法乙腈沉淀法处理样品，以伊马替尼为内标，Waters Acquity BEH C₁₈色谱柱（2.1 mm×100 mm，1.7 μm），流动相为0.1%甲酸水和乙腈。流速为0.3 mL·min^-1，柱温35℃。质谱条件为电喷雾电离源（ESI），检测方式为正离子电离、多离子反应监测（MRM）检测。结果阿西替尼血药浓度在0.1~100 ng·mL^-1内线性关系良好（r=0.999 6），定量下限为0.1 ng·mL^-1。日内、日间精密度RSD<5.56%，提取回收率>87.87%。大鼠血浆中的阿西替尼在室温、4℃，-80℃，12 h后以及反复冻融3次后均有良好的稳定性，且不存在基质效应。结论建立的测定阿西替尼血药浓度的方法准确、简单、快速，可以为阿西替尼的临床研究提供实验参考和依据。

关键词: 阿西替尼超高效液相色谱串联质谱法静脉给药

DOI：10.13748/j.cnki.issn1007-7693.2017.09.019

分类号:R917.101

基金项目:

Study on Plasma Concentration and Pharmacokinetics of Axitinib After Intravenous Administration in Rats by UPLC-MS/MS

FENG Yanlin, HONG Yan, TIAN Weiqiang

Department of Phmarcy, the Fifth Affiliated Hospital of Wenzhou Medical University, Lishui Municipal Central Hospital, Lishui 323000, China

Abstract:

OBJECTIVE To develop a ultra high-performance liquid chromatography-tandem mass spectrometry separation method(UPLC-MS/MS) for the pharmacokinetic study of Axitinib after intravenous administration. METHODS Plasma samples were treated by acetonitrile precipitation. The effective UPLC-MS/MS separation of the examined compounds was applied on an Acquity BEH C₁₈ column (2.1 mm×50 mm, 1.7 μm) column with a gradient mobile phase system consisting of 0.1% formic acid in water and acetonitrile. The analysis was performed with a flow rate of 0.3 mL·min^-1. An electrospray ionization (ESI) was used to detect in a positive ion mode. The scanning mode was MRM. RESULTS The assay was validated over concentration ranges of 0.1-100 ng·mL^-1, with a lower limit of quantification (LLOQ) of 0.1 ng·mL^-1. Intra-and inter-assay precision values for replicate quality control samples were within 5.56%. Assay recoveries of Axitinib was higher than 87.87%. Axitinib were stable in rat plasma for at least 24 h at room temperature, 30 days at 4℃ and -20℃, and following at least three freeze-thaw cycles. Furthermore, no notable matrix effect was observed for Axitinib. CONCLUSION The accurate and simple method developed can be provided the basis and applied to clinical pharmacokinetic study.

Key words: Axitinib UPLC-MS/MS intravenous administration