8-Substituted, syn-Configured Adenosine Derivatives as Potential Inhibitors of the Enzyme IspE from the Non-Mevalonate Pathway of Isoprenoid Biosynthesis

8-Substituted, syn-Configured Adenosine Derivatives as Potential Inhibitors of the Enzyme IspE from the Non-Mevalonate Pathway of Isoprenoid Biosynthesis

The enzymes of the non‐mevalonate pathway for isoprenoid biosynthesis are attractive targets for drugs against various diseases, including malaria. We describe herein the structure‐based design, synthesis, conformational analysis, and biological evaluation of several 8‐brominated or 8‐aminated adeno...

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Veröffentlicht in:European journal of organic chemistry 2015-11, Vol.2015 (33), p.7276-7286
Hauptverfasser: Harder, Michael, Schäfer, Elisabeth, Kümin, Tobias, Illarionov, Boris, Bacher, Adelbert, Fischer, Markus, Diederich, François, Bernet, Bruno
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Bacteriology
Binding sites
Biosynthesis
Conformation analysis
Enzymes
Hydrogen bonds
Inhibitors
Medicinal chemistry
Nucleosides
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container_end_page 7286
container_issue 33
container_start_page 7276
container_title European journal of organic chemistry
container_volume 2015
creator Harder, Michael
Schäfer, Elisabeth
Kümin, Tobias
Illarionov, Boris
Bacher, Adelbert
Fischer, Markus
Diederich, François
Bernet, Bruno
description The enzymes of the non‐mevalonate pathway for isoprenoid biosynthesis are attractive targets for drugs against various diseases, including malaria. We describe herein the structure‐based design, synthesis, conformational analysis, and biological evaluation of several 8‐brominated or 8‐aminated adenosine derivatives with different substituents at C(5′), targeting the ATP‐adenine binding site of the IspE protein from the non‐mevalonate pathway. An exhaustive conformational analysis of the adenosine derivatives both in solution and in the solid state confirmed the desired syn orientation of the adenine moiety. Despite this favorable pre‐organization for binding to the cofactor pocket, biological evaluation of the inhibitors showed only a very modest inhibitory activity. A structure‐based design approach has been used to develop 8‐bromo‐ and 8‐amino‐adenosine‐derived inhibitors with different substituents at C(5′), targeting the ATP‐binding pocket of the enzyme IspE. An exhaustive conformational analysis in the solid state and in solution was performed and the biological activities evaluated. The new adenosine derivatives were found to be weakly binding ligands.
doi_str_mv 10.1002/ejoc.201501150
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subjects Bacteriology
Binding sites
Biosynthesis
Conformation analysis
Enzymes
Hydrogen bonds
Inhibitors
Medicinal chemistry
Nucleosides
title 8-Substituted, syn-Configured Adenosine Derivatives as Potential Inhibitors of the Enzyme IspE from the Non-Mevalonate Pathway of Isoprenoid Biosynthesis
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