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Ting, L; Shi, W; Lewandowicz, A; Singh, V; Mwakingwe, A; Birck, M R; Taylor Ringia, E A; Bench, G; Madrid, D C; Tyler, P C; Evans, G B; Furneaux, R H; Schramm, V L; Kim, K.
Lawrence Livermore National Lab., Livermore, CA (United States). Funding organisation: US Department of Energy (United States)2004
Lawrence Livermore National Lab., Livermore, CA (United States). Funding organisation: US Department of Energy (United States)2004
AbstractAbstract
[en] Plasmodium falciparum is unable to synthesize purine bases and relies upon purine salvage and purine recycling to meet its purine needs. We report that purines formed as products of the polyamine pathway are recycled in a novel pathway in which 5'-methylthioinosine is generated by adenosine deaminase. The action of P. falciparum purine nucleoside phosphorylase is a convergent step of purine salvage, converting both 5'-methylthioinosine and inosine to hypoxanthine. We used accelerator mass spectrometry to verify that 5'-methylthioinosine is an active nucleic acid precursor in P. falciparum. Prior studies have shown that inhibitors of purine salvage enzymes kill malaria, but potent malaria-specific inhibitors of these enzymes have not previously been described. 5'-methylthio-Immucillin-H, a transition state analogue inhibitor that is selective for malarial over human purine nucleoside phosphorylase, kills P. falciparum in culture. Immucillins are currently in clinical trials for other indications and may have application as antimalarials
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UCRL-JRNL--204238; W-7405-ENG-48; Publication date March 14, 2005; PDF-FILE: 27; SIZE: 0.4 Megabytes
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Journal Article
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ANIMALS, AROMATICS, AZAARENES, DISEASES, ENZYMES, HETEROCYCLIC COMPOUNDS, HYDROXY COMPOUNDS, INFECTIOUS DISEASES, INVERTEBRATES, MICROORGANISMS, NUCLEOSIDES, NUCLEOTIDES, ORGANIC COMPOUNDS, ORGANIC NITROGEN COMPOUNDS, PARASITES, PARASITIC DISEASES, PHOSPHORUS-GROUP TRANSFERASES, PROTEINS, PROTOZOA, PURINES, RIBOSIDES, SPECTROSCOPY, SPOROZOA, TESTING, TRANSFERASES
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