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Development of Un-targeted Screening Method for Detection of Synthetic PDE-5 Inhibitors and Analogues Adulterated in Health Supplements on LCMS-IT-TOF

Posters | 2015 | ShimadzuInstrumentation
LC/TOF, LC/MS, LC/MS/MS, LC/IT
Industries
Pharma & Biopharma
Manufacturer
Shimadzu

Summary

Importance of the Topic


Adulteration of health supplements with unapproved synthetic PDE-5 inhibitors and their analogues poses serious health risks and regulatory challenges. Conventional targeted methods may miss unknown adulterants, highlighting the need for high-resolution untargeted screening.

Objectives and Study Overview


The study aimed to establish an untargeted LCMS-IT-TOF screening workflow using a compound database and MetID software. Thirty-two known PDE-5 inhibitors and analogues were used to evaluate method performance in five locally sourced supplements.

Methodology and Instrumentation


Sample Preparation:
  • Capsule contents extracted with methanol (1 g in 10 mL)
  • Sonication for 20 min, filtration (0.2 µm PTFE)

Chromatography:
  • Shim-pack C18 column (150×2.0 mm, 5 µm)
  • Mobile phases A: water + 0.1% formic acid, B: acetonitrile + 0.1% formic acid
  • Gradient: 10% B → 75% B (0–20 min) → 10% B (20–25 min)

Mass Spectrometry:
  • LCMS-IT-TOF high-resolution mass spectrometer with ESI in positive mode
  • Multi-event TIC acquisition divided into 50 Da windows covering m/z 200–600
  • MetID Solution software for peak detection and database search (±5 ppm mass error)

Used Instrumentation


  • Shimadzu UFLC system
  • LCMS-IT-TOF mass spectrometer
  • Shim-pack C18 analytical column
  • Electrospray ionization (ESI) source

Results and Discussion


  • Multi-event vs. single-event: multi-event TIC showed approximately 2× higher peak areas for 32 analytes.
  • All 32 compounds were detected at 0.5 ppm in five supplement matrices using untargeted screening.
  • Core-structure search enabled identification of tadalafil analogues not present in the original database.
  • Matrix effects varied widely by sample and analyte, with some compounds showing strong suppression.
  • A tentative detection limit of 0.5 ppm was established for reliable untargeted screening under current conditions.

Benefits and Practical Applications


This workflow enables comprehensive monitoring of both known and emerging PDE-5 analogues in dietary supplements, supporting regulatory compliance, consumer safety, and QA/QC in pharmaceutical and nutraceutical laboratories.

Future Trends and Potential Applications


  • Expansion of compound libraries to include other adulterant classes and novel analogues
  • Integration of machine-learning algorithms for automated candidate prioritization
  • Extension to broader illicit compound screening (e.g., weight-loss drugs, stimulants)
  • Coupling with metabolomic profiling for holistic safety assessment

Conclusion


An untargeted LCMS-IT-TOF method with multi-event acquisition and MetID database matching was developed and validated for detecting synthetic PDE-5 inhibitors in health supplements, offering improved sensitivity, broad coverage of analogues, and a practical screening limit of 0.5 ppm.

References


  • B.J. Venhuis et al. J. Pharm. Biomed. Anal. 69 (2012) 196–208
  • D.N. Patel et al. J. Pharm. Biomed. Anal. 87 (2014) 176–190
  • J.H. Lee et al. Food Addit. Contam. A 30(11) (2013) 1849–1857

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