N-Oxygenation of Oxycodone and Retro-reduction of Oxycodone N-Oxide

N-Oxygenation of Oxycodone and Retro-reduction of Oxycodone N-Oxide

Oxycodone is used as a potent analgesic medication. Oxycodone is extensively metabolized. To fully describe its metabolism, the oxygenation of oxycodone to oxycodone N-oxide was investigated in hepatic preparations. The hypothesis tested was that oxycodone N-oxygenation was enzymatic and the amount...

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Veröffentlicht in:Drug metabolism and disposition 2020-02, Vol.48 (2), p.106-115
Hauptverfasser: Cashman, John R., Gohdes, Mark, de Kater, Annelies, Schoenhard, Grant
Format: Artikel
Sprache:eng
Schlagworte:
Aldehyde oxidase
Aldehydes
Cytochrome
Cytochromes
Demethylation
Dimethylaniline monooxygenase (N-oxide-forming)
Flavin
Hemoglobin
Hypotheses
In vivo methods and tests
Liver
Metabolism
Metabolites
NADP
Organic chemistry
Oxycodone
Oxygenation
Quinones
Reductase
Reductases
Reduction
Urine
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Zusammenfassung:Oxycodone is used as a potent analgesic medication. Oxycodone is extensively metabolized. To fully describe its metabolism, the oxygenation of oxycodone to oxycodone N-oxide was investigated in hepatic preparations. The hypothesis tested was that oxycodone N-oxygenation was enzymatic and the amount of N-oxide detected was a consequence of both oxygenation and retro-reduction. Methods for testing the hypothesis included both in vitro and in vivo studies. Results indicated that oxycodone was N-oxygenated by the flavin-containing monooxygenase. Oxycodone N-oxide is chemically quite stable but in the presence of hepatic preparations and NADPH was retro-reduced to its parent compound oxycodone. Subsequently, oxycodone was metabolized to other metabolites including noroxycodone, noroxymorphone, and oxymorphone via cytochrome P-450. Retro-reduction of oxycodone N-oxide to oxycodone was facilitated by quinone reductase, aldehyde oxidase, and hemoglobin but not to a great extent by cytochrome P-450 or the flavin-containing monooxygenase. To confirm the in vitro observations, oxycodone was administered to rats and humans. In good agreement with in vitro results, substantial oxycodone N-oxide was observed in urine after oxycodone administration to rats and humans. Administration of oxycodone N-oxide to rats showed substantial amount of recovered oxycodone N-oxide. In vivo, noroxycodone was formed as a major rat urinary metabolite from oxycodone N-oxide presumably after retro-reduction to oxycodone and oxidative N-demethylation. To a lesser extent, oxycodone, noroxymorphone, and oxymorphone were observed as urinary metabolites. This manuscript describes the N-oxygenation of oxycodone in vitro as well as in small animals and humans. A new metabolite was quantified as oxycodone N-oxide. Oxycodone N-oxide undergoes extensive retro-reduction to oxycodone. This re-establishes the metabolic profile of oxycodone and introduces new concepts about a metabolic futile cycle related to oxycodone metabolism.
ISSN:0090-9556
1521-009X
DOI:10.1124/dmd.119.089300