Endocrine Connections (Feb 2019)

Discordance between testosterone measurement methods in castrated prostate cancer patients

  • Mélanie Rouleau,
  • Francis Lemire,
  • Michel Déry,
  • Benoît Thériault,
  • Gabriel Dubois,
  • Yves Fradet,
  • Paul Toren,
  • Chantal Guillemette,
  • Louis Lacombe,
  • Laurence Klotz,
  • Fred Saad,
  • Dominique Guérette,
  • Frédéric Pouliot

DOI
https://doi.org/10.1530/EC-18-0476
Journal volume & issue
Vol. 8, no. 2
pp. 132 – 140

Abstract

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Failure to suppress testosterone below 0.7 nM in castrated prostate cancer patients is associated with poor clinical outcomes. Testosterone levels in castrated patients are therefore routinely measured. Although mass spectrometry is the gold standard used to measure testosterone, most hospitals use an immunoassay method. In this study, we sought to evaluate the accuracy of an immunoassay method to measure castrate testosterone levels, with mass spectrometry as the reference standard. We retrospectively evaluated a cohort of 435 serum samples retrieved from castrated prostate cancer patients from April to September 2017. No follow-up of clinical outcomes was performed. Serum testosterone levels were measured in the same sample using liquid chromatography coupled with tandem mass spectrometry and electrochemiluminescent immunoassay methods. The mean testosterone levels were significantly higher with immunoassay than with mass spectrometry (0.672 ± 0.359 vs 0.461 ± 0.541 nM; P 0.7 nM was significantly higher with immunoassay (22.1%) than with mass spectrometry (13.1%; P 0.7 nM by immunoassay can result in an inaccurately identified castration status. Suboptimal testosterone levels in castrated patients should be confirmed by either mass spectrometry or an immunoassay method validated at low testosterone levels and interpreted with caution before any changes are made to treatment management.

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