Evaluation of dermorphin metabolism using zebrafish water tank model and human liver microsomes.
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2021
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Background: Dermorphin is a heptapeptide with an analgesic potential higher than morphine that does not
present the same risk for the development of tolerance. These pharmacological features make dermorphin a potential
doping agent in competitive sports and it is already prohibited for racehorses. For athletes, the development of an
efficient strategy to monitor for its abuse necessitates an investigation of the metabolism of dermorphin in humans.
Methods: Here, human liver microsomes and zebrafish were utilized as model systems of human metabolism to
evaluate the presence and kinetics of metabolites derived from dermorphin. Five hours after its administration, the
presence of dermorphin metabolites could be detected in both models by liquid chromatography coupled to high-
resolution mass spectrometry.
Results: Although the two models showed common results, marked differences were also observed in relation to the
formed metabolites. Six putative metabolites, based on their exact masses of m/z 479.1915, m/z 501.1733, m/z
495.1657, m/z 223.1073, m/z 180.1017 and m/z 457.2085, are proposed to represent the metabolic pattern of dermor-
phin. The major metabolite generated from the administration of dermorphin in both models was YAFG-OH (m/z
457.2085), which is the N-terminal tetrapeptide previously identified from studies on rats.
Conclusion: Its extensive characterization and commercial availability suggest that it could serve as a primary target
analyte for the detection of dermorphin misuse. The metabolomics approach also allowed the assignment of other
confirmatory metabolites.
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Doping analysis, Chromatography
Citação
CASTRO, J. de L. et al. Evaluation of dermorphin metabolism using zebrafish water tank model and human liver microsomes. Current Drug Metabolism, v. 22, p. 372-382, 2021. Disponível em: <https://www.eurekaselect.com/article/114239>. Acesso em: 11 out. 2022.