Structure-activity analysis of CJ-15,801 analogues that interact with Plasmodium falciparum pantothenate kinase and inhibit parasite proliferation

dc.contributor.authorSpry, Christina
dc.contributor.authorSewell, Alan L
dc.contributor.authorHering, Yuliya
dc.contributor.authorVilla, Mathew V J
dc.contributor.authorWeber, Jonas
dc.contributor.authorHobson, Stephen J
dc.contributor.authorHarnor, Suzannah J
dc.contributor.authorGul, Sheraz
dc.contributor.authorMarquez, Rodolfo
dc.contributor.authorSaliba, Kevin J
dc.date.accessioned2018-01-09T01:44:55Z
dc.date.issued2018-01-01
dc.description.abstractSurvival of the human malaria parasite Plasmodium falciparum is dependent on pantothenate (vitamin B5), a precursor of the fundamental enzyme cofactor coenzyme A. CJ-15,801, an enamide analogue of pantothenate isolated from the fungus Seimatosporium sp. CL28611, was previously shown to inhibit P. falciparum proliferation in vitro by targeting pantothenate utilization. To inform the design of next generation analogues, we set out to synthesize and test a series of synthetic enamide-bearing pantothenate analogues. We demonstrate that conservation of the R-pantoyl moiety and the trans-substituted double bond of CJ-15,801 is important for the selective, on-target antiplasmodial effect, while replacement of the carboxyl group is permitted, and, in one case, favored. Additionally, we show that the antiplasmodial potency of CJ-15,801 analogues that retain the R-pantoyl and trans-substituted enamide moieties correlates with inhibition of P. falciparum pantothenate kinase (PfPanK)-catalyzed pantothenate phosphorylation, implicating the interaction with PfPanK as a key determinant of antiplasmodial activity.en_AU
dc.description.sponsorshipC.S. was funded by an NHMRC Overseas Biomedical Fellowship (1016357). EPSRC and Syngenta provided postgraduate support (MJV) and a Leadership Fellowship (RM). Additional support was provided by Dr. Ian Sword, the EPSRC (grant EP/H005692/1) and the COST Action CM0801.en_AU
dc.format.mimetypeapplication/pdfen_AU
dc.identifier.issn0223-5234en_AU
dc.identifier.urihttp://hdl.handle.net/1885/139108
dc.publisherElsevieren_AU
dc.relationhttp://purl.org/au-research/grants/nhmrc/1016357en_AU
dc.rights© 2017 Elsevier B.V. http://www.sherpa.ac.uk/romeo/issn/0223-5234/..."Author's post-print on open access repository after an embargo period of between 12 months and 48 months" from SHERPA/RoMEO site (as at 9/01/18).en_AU
dc.sourceEuropean journal of medicinal chemistryen_AU
dc.subjectantimalarialen_AU
dc.subjectcj-15,801en_AU
dc.subjectpantothenateen_AU
dc.subjectpantothenate kinaseen_AU
dc.subjectplasmodium falciparumen_AU
dc.subjectantimalarialsen_AU
dc.subjectcell proliferationen_AU
dc.subjectdose-response relationship, drugen_AU
dc.subjecthumansen_AU
dc.subjectmolecular structureen_AU
dc.subjectpantothenic aciden_AU
dc.subjectparasitic sensitivity testsen_AU
dc.subjectphosphotransferases (alcohol group acceptor)en_AU
dc.subjectplasmodium falciparumen_AU
dc.subjectstructure-activity relationshipen_AU
dc.titleStructure-activity analysis of CJ-15,801 analogues that interact with Plasmodium falciparum pantothenate kinase and inhibit parasite proliferationen_AU
dc.typeJournal articleen_AU
dcterms.accessRightsOpen Accessen_AU
local.bibliographicCitation.lastpage1147en_AU
local.bibliographicCitation.startpage1139en_AU
local.contributor.affiliationSpry, C., Research School of Biology, The Australian National Universityen_AU
local.contributor.affiliationSaliba, K. J., Medical School, College of Medicine, Biology and Environment, The Australian National Universityen_AU
local.contributor.authoruidu3359155en_AU
local.identifier.ariespublicationa383154xPUB9197
local.identifier.citationvolume143en_AU
local.identifier.doi10.1016/j.ejmech.2017.08.050en_AU
local.identifier.essn1768-3254en_AU
local.publisher.urlhttps://www.elsevier.com/en_AU
local.type.statusAccepted Versionen_AU

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