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dc.contributor.authorGibhard, L.
dc.contributor.authorCoertzen, D.
dc.contributor.authorReader, J.
dc.contributor.authorvan der Watt, M.E.
dc.contributor.authorBirkholtz, L.M.
dc.contributor.authorWong, H.N.
dc.contributor.authorBatty, Kevin
dc.contributor.authorHaynes, R.K.
dc.contributor.authorWiesner, L.
dc.date.accessioned2022-07-18T04:42:41Z
dc.date.available2022-07-18T04:42:41Z
dc.date.issued2021
dc.identifier.citationGibhard, L. and Coertzen, D. and Reader, J. and van der Watt, M.E. and Birkholtz, L.M. and Wong, H.N. and Batty, K.T. et al. 2021. The artemiside-artemisox-artemisone-m1 tetrad: Efficacies against blood stage p. falciparum parasites, dmpk properties, and the case for artemiside. Pharmaceutics. 13 (12): ARTN 2066.
dc.identifier.urihttp://hdl.handle.net/20.500.11937/88951
dc.identifier.doi10.3390/pharmaceutics13122066
dc.description.abstract

Because of the need to replace the current clinical artemisinins in artemisinin combination therapies, we are evaluating fitness of amino-artemisinins for this purpose. These include the thiomorpholine derivative artemiside obtained in one scalable synthetic step from dihydroartemisinin (DHA) and the derived sulfone artemisone. We have recently shown that artemiside undergoes facile metabolism via the sulfoxide artemisox into artemisone and thence into the unsaturated metabolite M1; DHA is not a metabolite. Artemisox and M1 are now found to be approximately equipotent with artemiside and artemisone in vitro against asexual P. falciparum (Pf ) blood stage parasites (IC50 1.5–2.6 nM). Against Pf NF54 blood stage gametocytes, artemisox is potently active (IC50 18.9 nM early-stage, 2.7 nM late-stage), although against the late-stage gametocytes, activity is expressed, like other amino-artemisinins, at a prolonged incubation time of 72 h. Comparative drug metabolism and pharmacokinetic (DMPK) properties were assessed via po and iv administration of artemiside, artemisox, and artemisone in a murine model. Following oral administration, the composite Cmax value of artemiside plus its metabolites artemisox and artemisone formed in vivo is some 2.6-fold higher than that attained following administration of artemisone alone. Given that efficacy of short half-life rapidly-acting antimalarial drugs such as the artemisinins is associated with Cmax, it is apparent that artemiside will be more active than artemisone in vivo, due to additive effects of the metabolites. As is evident from earlier data, artemiside indeed possesses appreciably greater efficacy in vivo against murine malaria. Overall, the higher exposure levels of active drug following administration of artemiside coupled with its synthetic accessibility indicate it is much the preferred drug for incorporation into rational new artemisinin combination therapies.

dc.languageEnglish
dc.publisherMDPI
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/
dc.subjectScience & Technology
dc.subjectLife Sciences & Biomedicine
dc.subjectPharmacology & Pharmacy
dc.subjectantimalarial drugs
dc.subjectartemisinins
dc.subjectACTs
dc.subjectresistance
dc.subjectamino-artemisinins
dc.subjectpharmacokinetics
dc.subjectmetabolism
dc.subjectC-max
dc.subjectdrug efficacy
dc.subjectHIGH-THROUGHPUT ASSAY
dc.subjectANTIMALARIAL-DRUG
dc.subjectDIHYDROARTEMISININ
dc.subjectPHARMACOKINETICS
dc.subjectARTESUNATE
dc.subjectRESISTANCE
dc.subjectMALARIA
dc.subjectBIOAVAILABILITY
dc.subjectSUSCEPTIBILITY
dc.subjectCOMBINATION
dc.titleThe artemiside-artemisox-artemisone-m1 tetrad: Efficacies against blood stage p. falciparum parasites, dmpk properties, and the case for artemiside
dc.typeJournal Article
dcterms.source.volume13
dcterms.source.number12
dcterms.source.issn1999-4923
dcterms.source.titlePharmaceutics
dc.date.updated2022-07-18T04:42:38Z
curtin.departmentCurtin Medical School
curtin.accessStatusOpen access
curtin.facultyFaculty of Health Sciences
curtin.contributor.orcidBatty, Kevin [0000-0003-3850-1778]
curtin.identifier.article-numberARTN 2066
dcterms.source.eissn1999-4923
curtin.contributor.scopusauthoridBatty, Kevin [7004366064]


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