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Malaria Journal
Published in: Malaria Journal 1/2014

Open Access 01-12-2014 | Research

Enantioselective metabolism of primaquine by human CYP2D6

Authors: Pius S Fasinu, Babu L Tekwani, NP Dhammika Nanayakkara, Bharathi Avula, HMT Bandara Herath, Yan-Hong Wang, Vijender R Adelli, Mahmoud A Elsohly, Shabana I Khan, Ikhlas A Khan, Brandon S Pybus, Sean R Marcsisin, Gregory A Reichard, James D McChesney, Larry A Walker

Published in: Malaria Journal | Issue 1/2014

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Abstract

Background

Primaquine, currently the only approved drug for the treatment and radical cure of Plasmodium vivax malaria, is still used as a racemic mixture. Clinical use of primaquine has been limited due to haemolytic toxicity in individuals with genetic deficiency in glucose-6-phosphate dehydrogenase. Earlier studies have linked its therapeutic effects to CYP2D6-generated metabolites. The aim of the current study was to investigate the differential generation of the CYP2D6 metabolites by racemic primaquine and its individual enantiomers.

Methods

Stable isotope 13C-labelled primaquine and its two enantiomers were incubated with recombinant cytochrome-P450 supersomes containing CYP2D6 under optimized conditions. Metabolite identification and time-point quantitative analysis were performed using LC-MS/MS. UHPLC retention time, twin peaks with a mass difference of 6, MS-MS fragmentation pattern, and relative peak area with respect to parent compound were used for phenotyping and quantitative analysis of metabolites.

Results

The rate of metabolism of (+)-(S)-primaquine was significantly higher (50% depletion of 20 μM in 120 min) compared to (−)-(R)-primaquine (30% depletion) when incubated with CYP2D6. The estimated V max (μmol/min/mg) were 0.75, 0.98 and 0.42, with K m (μM) of 24.2, 33.1 and 21.6 for (±)-primaquine, (+)-primaquine and (−)-primaquine, respectively. Three stable mono-hydroxylated metabolites, namely, 2-, 3- and 4-hydroxyprimaquine (2-OH-PQ, 3-OH-PQ, and 4-OH-PQ), were identified and quantified. 2-OH-PQ was preferentially formed from (+)-primaquine in a ratio of 4:1 compared to (−)-primaquine. The racemic (±)-primaquine showed a pattern similar to the (−)-primaquine; 2-OH-PQ accounted for about 15–17% of total CYP2D6-mediated conversion of (+)-primaquine. In contrast, 4-OH-PQ was preferentially formed with (−)-primaquine (5:1), accounting for 22% of the total (−)-primaquine conversion. 3-OH-PQ was generated from both enantiomers and racemate. 5-hydroxyprimaquine was unstable. Its orthoquinone degradation product (twice as abundant in (+)-primaquine compared to (−)-primaquine) was identified and accounted for 18–20% of the CYP2D6-mediated conversion of (+)-primaquine. Other minor metabolites included dihydroxyprimaquine species, two quinone-imine products of dihydroxylated primaquine, and a primaquine terminal alcohol with variable generation from the individual enantiomers.

Conclusion

The metabolism of primaquine by human CYP2D6 and the generation of its metabolites display enantio-selectivity regarding formation of hydroxylated product profiles. This may partly explain differential pharmacologic and toxicologic properties of primaquine enantiomers.
Appendix
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Metadata
Title
Enantioselective metabolism of primaquine by human CYP2D6
Authors
Pius S Fasinu
Babu L Tekwani
NP Dhammika Nanayakkara
Bharathi Avula
HMT Bandara Herath
Yan-Hong Wang
Vijender R Adelli
Mahmoud A Elsohly
Shabana I Khan
Ikhlas A Khan
Brandon S Pybus
Sean R Marcsisin
Gregory A Reichard
James D McChesney
Larry A Walker
Publication date
01-12-2014
Publisher
BioMed Central
Published in
Malaria Journal / Issue 1/2014
Electronic ISSN: 1475-2875
DOI
https://doi.org/10.1186/1475-2875-13-507

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