Enantioselective Interactions of Anti-Infective 8-Aminoquinoline Therapeutics with Human Monoamine Oxidases A and B

Chaurasiya, Narayan D.; Liu, Haining; Doerksen, Robert J.; Nanayakkara, N. P. Dhammika; Walker, Larry; Tekwani, Babu L.

doi:10.3390/ph14050398

Cited by 4 publications

(2 citation statements)

References 76 publications

(121 reference statements)

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“…The differential pharmacokinetic, metabolism and pharmacologic profiles of individual enantiomers of PQ is now well established, as evidenced in in vitro human hepatocytes and also in animals ( Fasinu et al, 2014 ; 2016 ; 2022 ; Saunders et al, 2014 ; Chaurasiya et al, 2021 ). A recent study from our group also demonstrated highly enantioselective PK and metabolism profiles in subjects treated with single dose of individual PQ enantiomers ( Khan et al, 2022a ).…”

Section: Discussionmentioning

confidence: 99%

“…With respect to metabolism, as observed in our single dose study ( Khan et al, 2022a ), plasma exposure to parent drug was significantly higher for SPQ treated groups than for RPQ, and RSPQ behaved in an additive fashion. Plasma cPQ levels were much higher after RPQ administration than SPQ, likely reflecting the greater vulnerability of RPQ to metabolism by monoamine oxidases ( Chaurasiya et al, 2021 ). This presumably also accounts for the reduced exposure to the parent drug after RPQ administration.…”

Section: Discussionmentioning

confidence: 99%

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Comparative metabolism and tolerability of racemic primaquine and its enantiomers in human volunteers during 7-day administration

et al. 2023

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Primaquine (PQ) is an 8-aminoquinoline antimalarial, active against dormant Plasmodium vivax hypnozoites and P. falciparum mature gametocytes. PQ is currently used for P. vivax radical cure and prevention of malaria transmission. PQ is a racemic drug and since the metabolism and pharmacology of PQ’s enantiomers have been shown to be divergent, the objectives of this study were to evaluate the comparative tolerability and metabolism of PQ with respect to its two enantiomers in human volunteers in a 7 days’ treatment schedule. Fifteen subjects with normal glucose-6-phosphate dehydrogenase (G6PDn) completed four arms, receiving each of the treatments, once daily for 7 days, in a crossover fashion, with a 7–14 days washout period in between: R-(−) enantiomer (RPQ) 22.5 mg; S-(+) enantiomer (SPQ) 22.5 mg; racemic PQ (RSPQ) 45 mg, and placebo. Volunteers were monitored for any adverse events (AEs) during the study period. PQ and metabolites were quantified in plasma and red blood cells (RBCs) by UHPLC-UV-MS/MS. Plasma PQ was significantly higher in SPQ treatment group than for RPQ. Carboxy-primaquine, a major plasma metabolite, was much higher in the RPQ treated group than SPQ; primaquine carbamoyl glucuronide, another major plasma metabolite, was derived only from SPQ. The ortho-quinone metabolites were also detected and showed differences for the two enantiomers in a similar pattern to the parent drugs. Both enantiomers and racemic PQ were well tolerated in G6PDn subjects with the 7 days regimen; three subjects showed mild AEs which did not require any intervention or discontinuation of the drug. The most consistent changes in G6PDn subjects were a gradual increase in methemoglobin and bilirubin, but these were not clinically important. However, the bilirubin increase suggests mild progressive damage to a small fraction of red cells. PQ enantiomers were also individually administered to two G6PD deficient (G6PDd) subjects, one heterozygous female and one hemizygous male. These G6PDd subjects showed similar results with the two enantiomers, but the responses in the hemizygous male were more pronounced. These studies suggest that although the metabolism profiles of individual PQ enantiomers are markedly different, they did not show significant differences in the safety and tolerability in G6PDn subjects.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Comparative metabolism and tolerability of racemic primaquine and its enantiomers in human volunteers during 7-day administration

et al. 2023

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Roles of selected non-P450 human oxidoreductase enzymes in protective and toxic effects of chemicals: review and compilation of reactions

Rendić¹,

Crouch

Guengerich

2022

Arch Toxicol

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This is an overview of the metabolic reactions of drugs, natural products, physiological compounds, and other (general) chemicals catalyzed by flavin monooxygenase (FMO), monoamine oxidase (MAO), NAD(P)H quinone oxidoreductase (NQO), and molybdenum hydroxylase enzymes (aldehyde oxidase (AOX) and xanthine oxidoreductase (XOR)), including roles as substrates, inducers, and inhibitors of the enzymes. The metabolism and bioactivation of selected examples of each group (i.e., drugs, “general chemicals,” natural products, and physiological compounds) are discussed. We identified a higher fraction of bioactivation reactions for FMO enzymes compared to other enzymes, predominately involving drugs and general chemicals. With MAO enzymes, physiological compounds predominate as substrates, and some products lead to unwanted side effects or illness. AOX and XOR enzymes are molybdenum hydroxylases that catalyze the oxidation of various heteroaromatic rings and aldehydes and the reduction of a number of different functional groups. While neither of these two enzymes contributes substantially to the metabolism of currently marketed drugs, AOX has become a frequently encountered route of metabolism among drug discovery programs in the past 10–15 years. XOR has even less of a role in the metabolism of clinical drugs and preclinical drug candidates than AOX, likely due to narrower substrate specificity.

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Comparative single dose pharmacokinetics and metabolism of racemic primaquine and its enantiomers in human volunteers

Khan

Wang

Chaurasiya

et al. 2022

Drug Metabolism and Pharmacokinetics

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Enantioselective Interactions of Anti-Infective 8-Aminoquinoline Therapeutics with Human Monoamine Oxidases A and B

Cited by 4 publications

References 76 publications

Comparative metabolism and tolerability of racemic primaquine and its enantiomers in human volunteers during 7-day administration

Comparative metabolism and tolerability of racemic primaquine and its enantiomers in human volunteers during 7-day administration

Roles of selected non-P450 human oxidoreductase enzymes in protective and toxic effects of chemicals: review and compilation of reactions

Comparative single dose pharmacokinetics and metabolism of racemic primaquine and its enantiomers in human volunteers

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