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Comparative pharmacokinetics and tissue distribution of primaquine enantiomers in mice.

Pius S FasinuNarayan D ChaurasiyaN P Dhammika NanayakkaraYan-Hong WangH M T Bandara HerathBharathi AvulaJames D McChesneyDavid JollowLarry A WalkerBabu L Tekwani
Published in: Malaria journal (2022)
These studies show that in mice, PQ enantiomers are differentially biodistributed and metabolized, which may contribute to differential pharmacologic and toxicity profiles of PQ enantiomers. The findings on higher levels of PQ-o-quinone in liver and RBCs compared to plasma and preferential generation of this metabolite from SPQ are consistent with the higher anti-malarial efficacy of SPQ observed in the mouse causal prophylaxis test, and higher haemolytic toxicity in the humanized mouse model of G6PD deficiency. Potential relevance of these findings to clinical use of racemic PQ and other 8-aminoquinolines vis-à-vis need for further clinical evaluation of individual enantiomers are discussed.
Keyphrases
  • mouse model
  • capillary electrophoresis
  • high fat diet induced
  • oxidative stress
  • mass spectrometry
  • metabolic syndrome
  • insulin resistance
  • skeletal muscle
  • monoclonal antibody