Exploring the transmission-blocking activity of antiplasmodial 3,6-diarylated imidazopyridazines

dc.contributor.authorCoertzen, Dina
dc.contributor.authorReader, Janette
dc.contributor.authorVan der Watt, Mariette Elizabeth
dc.contributor.authorLeshabane, Meta Kgaogelo
dc.contributor.authorLangeveld, Henrico
dc.contributor.authorCheuka, Peter M.
dc.contributor.authorDziwornu, Godwin Akpeko
dc.contributor.authorChibale, Kelly
dc.contributor.authorBirkholtz, Lyn-Marie
dc.contributor.emaildina.coertzen@up.ac.zaen_ZA
dc.date.accessioned2022-01-12T07:12:54Z
dc.date.issued2021
dc.description.abstractThe effectiveness of current antimalarial therapies that cure patients of the pathogenic asexual blood stages is rapidly declining due to the spread of antimalarial drug resistance. This requires the development of novel chemotypes curative for asexual blood stages but additionally, such chemotypes should also target the sexually differentiated gametocytes and thereby block disease transmission. Kinase inhibitors, specifically imidazopyridazines, were previously described as highly effective, dual-active compounds in vitro. However, amongst other shortcomings, poor solubility and cardiotoxicity risks prevented these compounds from being further developed. In a recent study, novel 3,6-diarylated imidazopyridazine derivatives showed improved solubility and a decrease in inhibition of the human ether-a-go-go-related gene (hERG), suggesting reduced cardiotoxicity risks, with potent sub-micromolar antiplasmodial activities. Here, we report the in vitro activity of these 3,6-diarylated imidazopyridazine derivates against both asexual blood and gametocyte stages of the human malaria parasite, Plasmodium falciparum, in vitro. We highlight several potentially dual-active compounds with nanomolar activities (IC50’s 0.7–104 nM) against both drug sensitive and resistant strains of P. falciparum with these compounds also displaying activity against transmissible gametocytes (IC50’s 1180.3–1787.5 nM). Taken together, the new generation 3,6-diarylated imidazopyridazines have potent activity against P. falciparum parasites in vitro with improved physicochemical and toxicity profiles.en_ZA
dc.description.departmentBiochemistryen_ZA
dc.description.departmentGeneticsen_ZA
dc.description.departmentMicrobiology and Plant Pathologyen_ZA
dc.description.departmentUP Centre for Sustainable Malaria Control (UP CSMC)en_ZA
dc.description.embargo2022-10-20
dc.description.librarianhj2022en_ZA
dc.description.sponsorshipThe South African Medical Research Council, the DST/NRF South African Research Chairs Initiative Grants and a Communities of Practice grant.en_ZA
dc.description.urihttps://www.tandfonline.com/loi/ttrs20en_ZA
dc.identifier.citationDina Coertzen, Janette Reader, Mariëtte E. van der Watt, Meta M. Leshabane, Henrico Langeveld, Peter M. Cheuka, Godwin A. Dziwornu, Kelly Chibale & Lyn-Marie Birkholtz (2021): Exploring the transmission-blocking activity of antiplasmodial 3,6-diarylated imidazopyridazines, Transactions of the Royal Society of South Africa, 76(3): 225-233, DOI: 10.1080/0035919X.2021.1982792.en_ZA
dc.identifier.issn0035-919X (print)
dc.identifier.issn2154-0098 (online)
dc.identifier.other10.1080/0035919X.2021.1982792
dc.identifier.urihttp://hdl.handle.net/2263/83297
dc.language.isoenen_ZA
dc.publisherTaylor and Francisen_ZA
dc.rights© 2021 Royal Society of South Africa. This is an electronic version of an article published in Transactions of the Royal Society of South Africa, vol. 76, no. 3, pp. 225-233, 2021, doi: 10.1080/0035919X.2021.1982792. Transactions of the Royal Society of South Africa is available online at : https://www.tandfonline.com/loi/ttrs20.en_ZA
dc.subjectMalariaen_ZA
dc.subjectKinase inhibitorsen_ZA
dc.subjectImidazopyridazinesen_ZA
dc.subjectAntiplasmodialen_ZA
dc.subjectAntimalarialsen_ZA
dc.subjectTransmission-blockingen_ZA
dc.subjectHuman ether-a-go-go-related gene (hERG)en_ZA
dc.titleExploring the transmission-blocking activity of antiplasmodial 3,6-diarylated imidazopyridazinesen_ZA
dc.typePostprint Articleen_ZA

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