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Offline and online sample extraction for the quantification of benzodiazepines in human plasma or serum for clinical research

Applications | 2017 | Thermo Fisher ScientificInstrumentation
Sample Preparation, LC/MS, LC/MS/MS, LC/QQQ
Industries
Clinical Research
Manufacturer
Thermo Fisher Scientific, RECIPE

Summary

Importance of Topic


The accurate quantification of benzodiazepines in human plasma and serum is critical for clinical research, therapeutic drug monitoring, toxicology screening, and pharmacokinetic studies. These compounds have a narrow therapeutic window and significant interindividual variability, making sensitive, selective, and reproducible methods essential to ensure reliable patient care and research outcomes.

Study Objectives and Overview


This work aimed to develop and validate a robust liquid chromatography–tandem mass spectrometry (LC-MS/MS) method for simultaneous quantification of 34 benzodiazepines and metabolites in human plasma or serum. Two sample-preparation workflows were compared: direct injection with automated internal standard addition and offline protein precipitation to enhance sensitivity.

Methodology and Instrumentation


  • Sample Types: Human plasma or serum, 50 µL aliquots.
  • Internal Standards: Twenty deuterated analogs added either online or offline.
  • Direct Injection Workflow: Automated internal standard addition in the autosampler followed by online solid-phase extraction (SPE) and LC separation.
  • Offline Protein Precipitation Workflow: Addition of internal standards to plasma or serum, followed by protein precipitation with organic solvent, vortex mixing, centrifugation, and transfer of supernatant.
  • Chromatography: SPE cartridge (online workflow) or direct injection (offline workflow), analytical column, gradient elution; run times of 8.5 min (direct) and 7.5 min (offline).
  • Mass Spectrometry: Thermo Scientific TSQ Endura triple quadrupole with heated electrospray ionization in positive mode; selected reaction monitoring (SRM) with two transitions per analyte for quantification and confirmation.
  • Data Acquisition and Processing: Thermo Scientific TraceFinder 3.3 software.

Results and Discussion


Linearity and Sensitivity
  • Calibrators covered typical clinical concentration ranges, with limits of quantification in the low ng/mL range.
  • Both workflows demonstrated linear response across calibration ranges and extended ranges via dilution up to 20-fold.
Accuracy and Precision
  • Accuracy bias between nominal and measured concentrations ranged from –7.3% to +15.6% (direct) and –7.3% to +12.4% (offline).
  • Intra-assay precision (%CV) was less than 14% for all analytes except zopiclone, which showed stability issues.
  • Inter-assay precision remained below 13% for all compounds except zopiclone in the offline workflow.
Chromatographic Performance
  • Representative chromatograms showed sharp, well-resolved peaks for the lowest calibrators.
  • Retention times were reproducible between runs and between workflows.

Benefits and Practical Applications


  • Flexibility: Choice of direct injection for high throughput or offline precipitation for enhanced sensitivity.
  • Comprehensive Panel: Simultaneous quantification of 34 analytes in a single run reduces sample volume and labor.
  • Minimal Sample Handling: Automated standard addition minimizes manual intervention and potential errors.
  • Clinical Research Utility: Suitable for pharmacokinetic studies, therapeutic drug monitoring, and toxicological investigations.

Future Trends and Possibilities


Advances in clinical and forensic toxicology will drive further integration of high-resolution mass spectrometry, micro-sampling techniques such as dried blood spots, and fully automated workflows. Expansion of analyte panels to include emerging designer benzodiazepines and active metabolites will be enabled by improvements in instrument sensitivity and software-driven data processing.

Conclusion


This LC-MS/MS method provides a validated, reliable, and flexible approach for quantifying a broad panel of benzodiazepines in human plasma or serum. Both direct injection and offline precipitation workflows meet stringent criteria for accuracy, precision, and linearity, supporting diverse clinical and research applications.

References


  • Thermo Fisher Scientific. Technical Note 64913, 2017.
  • RECIPE Chemicals + Instruments GmbH. ClinMass TDM Platform and Add-On Sets.

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