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Development and validation of an LC-MS/MS method for the bioanalysis of the major metamizole metabolites in human plasma.

Fabio BachmannLea BlaserManuel HaschkeStephan KrähenbühlUrs Duthaler
Published in: Bioanalysis (2020)
Aim: Metamizole is a frequently used antipyretic and analgesic prodrug, yet its pharmacokinetics has not been thoroughly studied in infants and with coadministered medications. Thus, an LC-MS/MS method was developed to quantify the four major metamizole metabolites in human plasma. Methodology: Pre- and postcolumn infusion was installed to enable robust analyte retention and electrospray ionization following deproteinization of plasma samples. Results: The method was linear (R > 0.996), accurate (93.1-106.0%) and precise (≤12.7%). Mean recovery was more than 91.8% and ion suppression less than 13.1% for all analytes. Pharmacokinetic profiles were reproducible after 4 years at -80°C except for the formylated metabolite (-22.2%). Conclusion: The method fulfilled pertinent criteria of validation guidelines and required only little sample volume. The method therefore qualifies for metamizole analyses in children.
Keyphrases
  • ms ms
  • low dose
  • young adults
  • spinal cord injury
  • cancer therapy
  • neuropathic pain
  • simultaneous determination