PHOSPHONATE ANALOGS OF CARBOCYCLIC PHOSPHORIBOSYLAMINE AND CARBOCYCLIC GLYCINAMIDE RIBONUCLEOTIDE |
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| Authors: | Robert Vince Mei Hua Carol A. Caperelli |
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| Affiliation: | 1. Department of Medicinal Chemistry College of Pharmacy , 308 Harvard St. S. E. University of Minnesota Minneapolis , MN 55455-0343;2. Division of Pharmaceutical Sciences College of Pharmacy , University of Cincinnati Medical Center Cincinnati , Ohio, 45267-0004 |
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| Abstract: | Abstract Analogs of intermediates in the de novo purine nucleotide biosynthetic pathway were synthesized to study the binding requirements of the corresponding enzymes. Because of the instability of the natural stubstrates, such as phosphoribosylamine, the use of the structurally stable phosphonate moiety and the carbocyclic ribose yields ideal analogs for these studies. In addition, these analogs can act as potential inhibitors of the de novo pathway leading to the design of anticancer agents. Enzyme studies with GAR synthetase and GAR transformylase reveal that the title compounds can act as substrates or inhibitors of the de novo enzymes. |
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