Detection of microdoses of rhEPO with the MAIIA test

The detection of recombinant human erythropoietin (rhEPO) is difficult and becomes more challenging when only microdoses are administered intravenously. Twenty‐three subjects were divided into two groups: EPO group (n = 7) and CONTROL group (n = 16). Seven urine and blood samples per subject were co...

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Bibliographic Details
Published in:Scandinavian journal of medicine & science in sports 2014-08, Vol.24 (4), p.634-641
Main Authors: Mørkeberg, J., Sharpe, K., Karstoft, K., Ashenden, M. J.
Format: Article
Language:English
Subjects:
Adult
blood passport
detection
doping
EPO
Erythropoietin - administration & dosage
Erythropoietin - blood
Erythropoietin - urine
Exercise - physiology
Humans
Male
Performance-Enhancing Substances - administration & dosage
Performance-Enhancing Substances - blood
Performance-Enhancing Substances - urine
Protein Isoforms - blood
Protein Isoforms - urine
Recombinant Proteins - administration & dosage
Recombinant Proteins - blood
Recombinant Proteins - urine
Sensitivity and Specificity
Substance Abuse Detection - methods
Young Adult
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Summary:The detection of recombinant human erythropoietin (rhEPO) is difficult and becomes more challenging when only microdoses are administered intravenously. Twenty‐three subjects were divided into two groups: EPO group (n = 7) and CONTROL group (n = 16). Seven urine and blood samples per subject were collected at least 5 days apart to determine within‐ and between‐subject standard deviations in the percentage of migrating isoforms by the MAIIA test. Six injections of 50 IU/kg bw (boosting dosage) of epoetin beta (Neorecormon, Roche Diagnostics, Hvidovre, Denmark) were performed intravenously during a 3‐week period, followed by two microinjections of only 10 IU/kg bw. Blood and urine samples were collected 2, 6, 12, and 72 h after the microinjection, as well as 72 h after the last boosting dose. Sensitivities and specificities of the MAIIA test were examined by absolute and passport thresholds. Sensitivity was 100% for at least 12 h after the microinjection, with ∼30% of plasma samples still exceeding the 99.9% passport threshold 72 h after a microinjection. The specificity was higher for the passport approach compared to the absolute approach, but there were no differences in sensitivities between approaches or between specimens (urine and plasma). We conclude that the MAIIA test shows potential for detecting very small doses of rhEPO.
ISSN:0905-7188
1600-0838
DOI:10.1111/sms.12049