Optimal 10-aminoartemisinins with potent transmission-blocking capabilities for new artemisinin combination therapies–activities against blood stage P. falciparum including PfKI3 C580Y mutants and liver stage P. berghei parasites
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| dc.contributor.author | Wong, Ho Ning
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| dc.contributor.author | Padin-Irizarry, Vivian
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| dc.contributor.author | Van der Watt, Mariette Elizabeth
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| dc.contributor.author | Reader, Janette
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| dc.contributor.author | Liebenberg, Wilna
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| dc.contributor.author | Wiesner, Lubbe
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| dc.contributor.author | Smith, Peter
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| dc.contributor.author | Eribez, Korina
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| dc.contributor.author | Winzeler, Elizabeth A.
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| dc.contributor.author | Kyle, Dennis E.
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| dc.contributor.author | Birkholtz, Lyn-Marie
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| dc.contributor.author | Coertzen, Dina
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| dc.contributor.author | Haynes, Richard K.
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| dc.date.accessioned | 2020-10-05T15:14:38Z | |
| dc.date.available | 2020-10-05T15:14:38Z | |
| dc.date.issued | 2020-01-10 | |
| dc.description | Supplementary Table 1 | In vitro activities of selected amino-artemisinins against liver stage P. berghei, dose response curves and cytotoxicities. | en_ZA |
| dc.description | Supplementary Material comprises experimental details for synthesis and characterization data of the amino-artemisinins, and dose response curves for the in vitro P. berghei sporozoite stage efficacy assays recorded in Excel format in CDD Vault: UCSD CDD_Vault_Export_RESULTS_KDE_03-25-2019. | en_ZA |
| dc.description.abstract | We have demonstrated previously that amino-artemisinins including artemiside and artemisone in which an amino group replaces the oxygen-bearing substituents attached to C-10 of the current clinical artemisinin derivatives dihydroartemisinin (DHA), artemether and artesunate, display potent activities in vitro against the asexual blood stages of Plasmodium falciparum (Pf ). In particular, the compounds are active against late blood stage Pf gametocytes, and are strongly synergistic in combination with the redox active drug methylene blue. In order to fortify the eventual selection of optimum amino-artemisinins for development into new triple combination therapies also active against artemisinin-resistant Pf mutants, we have prepared new amino-artemisinins based on the easily accessible and inexpensive DHA-piperazine. The latter was converted into alkyl- and aryl sulfonamides, ureas and amides. These derivatives were screened together with the comparator drugs DHA and the hitherto most active amino-artemisinins artemiside and artemisone against asexual and sexual blood stages of Pf and liver stage P. berghei (Pb) sporozoites. Several of the new amino-artemisinins bearing aryl-urea and -amide groups are potently active against both asexual, and late blood stage gametocytes (IC50 0.4-1.0 nM). Although the activities are superior to those of artemiside (IC50 1.5 nM) and artemisone (IC50 42.4 nM), the latter are more active against the liver stage Pb sporozoites (IC50 artemisone 28 nM). In addition, early results indicate these compounds tend not to display reduced susceptibility against parasites bearing the Pf Kelch 13 propeller domain C580Y mutation characteristic of artemisinin-resistant Pf. Thus, the advent of the amino-artemisinins including artemiside and artemisone will enable the development of new combination therapies that by virtue of the amino-artemisinin component itself will possess intrinsic transmission-blocking capabilities and may be effective against artemisinin resistant falciparum malaria. | en_ZA |
| dc.description.department | Biochemistry | en_ZA |
| dc.description.department | Genetics | en_ZA |
| dc.description.department | Microbiology and Plant Pathology | en_ZA |
| dc.description.librarian | am2020 | en_ZA |
| dc.description.sponsorship | This work was funded by the South African Medical Research Council (MRC) Flagship Project MALTB-Redox with funds from National Treasury under its Economic Competitiveness and Support Package to RH (MRC-RFA-UFSP-01-2013), the South African MRC Strategic Health Innovation Partnership (SHIP) grant, a South African MRC Collaborative Center for Malaria Research grant and South African National Research Foundation grants (UID 84627) to L-MB and to RH (UIDs 90682 and 98934). EW was supported by grants from the NIH (R01 AI090141-02), and Medicines for Malaria Venture, Geneva. | en_ZA |
| dc.description.uri | http://www.frontiersin.org/Chemistry | en_ZA |
| dc.identifier.citation | Wong HN, Padín-Irizarry V, van der Watt ME, Reader J, Liebenberg W, Wiesner L, Smith P, Eribez K, Winzeler EA, Kyle DE, Birkholtz L-M, Coertzen D and Haynes RK (2020) Optimal 10-Aminoartemisinins With Potent Transmission-Blocking Capabilities for New Artemisinin Combination Therapies–Activities Against Blood Stage P. falciparum Including PfKI3 C580Y Mutants and Liver Stage P. berghei Parasites. Frontiers in Chemistry 7:901. DOI: 10.3389/fchem.2019.00901 | en_ZA |
| dc.identifier.issn | 2296-2646 (online) | |
| dc.identifier.other | 10.3389/fchem.2019.00901 | |
| dc.identifier.uri | http://hdl.handle.net/2263/76347 | |
| dc.language.iso | en | en_ZA |
| dc.publisher | Frontiers Media | en_ZA |
| dc.rights | © 2020 Wong, Padín-Irizarry, van der Watt, Reader, Liebenberg, Wiesner, Smith, Eribez, Winzeler, Kyle, Birkholtz, Coertzen and Haynes. This is an open access article distributed under the terms of the Creative Commons Attribution License (CC BY). | en_ZA |
| dc.subject | Malaria | en_ZA |
| dc.subject | Gametocytes | en_ZA |
| dc.subject | Sporozoites | en_ZA |
| dc.subject | Amino-artemisinins | en_ZA |
| dc.subject | Transmission-blocking | en_ZA |
| dc.title | Optimal 10-aminoartemisinins with potent transmission-blocking capabilities for new artemisinin combination therapies–activities against blood stage P. falciparum including PfKI3 C580Y mutants and liver stage P. berghei parasites | en_ZA |
| dc.type | Article | en_ZA |
