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LC-MS/MS methods to quantify HCP002 in human plasma and urine: applications in a pharmacokinetic study.

Lu-Ning SunYe ZhangQiu-Chen FangYe ShenXue LiChao ChenHong-Wen ZhangYong-Qing Wang
Published in: Bioanalysis (2022)
Aim: HCP002, a phosphate-modified derivative of voriconazole, can improve solubility without using the nephrotoxic solubilizer, sulfobutylether-β-cyclodextrin. To study pharmacokinetics in humans, LC-MS/MS methods to quantify HCP002 in human plasma and urine were developed and validated. Method: After protein precipitation by acetonitrile containing voriconazole-d 3 , HCP002 was separated on a ZORBAX SB-Aq column, and LCMS/MS analysis was performed in multi-response monitoring mode. Results: The analytical run time was 3 min. Linearity was observed over the ranges of 0.100-40.0 and 0.400-200 μg/ml in plasma and urine, respectively. Precision and accuracy were within acceptable limits. Sample stability was confirmed. Conclusion: Rapid and reproducible methods quantified HCP002 in urine, and plasma samples were established.
Keyphrases
  • mass spectrometry
  • liquid chromatography
  • multiple sclerosis
  • ms ms
  • ionic liquid
  • high resolution
  • loop mediated isothermal amplification