Science & Justice
Volume 49, Issue 2 , Pages 102-106, June 2009

Detection of counterfeit antiviral drug Heptodin™ and classification of counterfeits using isotope amount ratio measurements by multicollector inductively coupled plasma mass spectrometry (MC-ICPMS) and isotope ratio mass spectrometry (IRMS)

  • Rebeca Santamaria-Fernandez

      Affiliations

    • LGC Ltd., Queens Road, Teddington, Middlesex, TW11 0LY, UK
    • Corresponding Author InformationCorresponding author.
    • ,
  • Ruth Hearn

      Affiliations

    • LGC Ltd., Queens Road, Teddington, Middlesex, TW11 0LY, UK
    • ,
  • Jean-Claude Wolff

      Affiliations

    • GlaxoSmithKline, Medicines Research Centre, Gunnels Wood Road, Stevenage, SG1 2NY, UK

Received 16 October 2008; received in revised form 19 December 2008; accepted 24 December 2008. published online 11 February 2009.

Abstract 

Isotope ratio mass spectrometry (IRMS) and multicollector inductively coupled plasma mass spectrometry (MC-ICP-MS) are highly important techniques that can provide forensic evidence that otherwise would not be available. MC-ICP-MS has proved to be a very powerful tool for measuring high precision and accuracy isotope amount ratios. In this work, the potential of combining isotope amount ratio measurements performed by MC-ICP-MS and IRMS for the detection of counterfeit pharmaceutical tablets has been investigated.

An extensive study for the antiviral drug Heptodin™ has been performed for several isotopic ratios combining MC-ICP-MS and an elemental analyser EA-IRMS for stable isotope amount ratio measurements. The study has been carried out for 139 batches of the antiviral drug and analyses have been performed for C, S, N and Mg isotope ratios. Authenticity ranges have been obtained for each isotopic system and combined to generate a unique multi-isotopic pattern only present in the genuine tablets. Counterfeit tablets have then been identified as those tablets with an isotopic fingerprint outside the genuine isotopic range.

The combination of those two techniques has therefore great potential for pharmaceutical counterfeit detection. A much greater power of discrimination is obtained when at least three isotopic systems are combined. The data from these studies could be presented as evidence in court and therefore methods need to be validated to support their credibility. It is also crucial to be able to produce uncertainty values associated to the isotope amount ratio measurements so that significant differences can be identified and the genuineness of a sample can be assessed.

Keywords: IRMS, Multicollector ICP-MS, Isotope ratio, Counterfeit drug, Authenticity, Forensic evidence

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PII: S1355-0306(08)00160-3

doi:10.1016/j.scijus.2008.12.003

Science & Justice
Volume 49, Issue 2 , Pages 102-106, June 2009

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