Potential Dental Biofilm Inhibitors: Dynamic Combinatorial Chemistry Affords Sugar-Based Molecules that Target Bacterial Glucosyltransferase
| Autor: | Evelien M Te Poele, Alwin M. Hartman, Lubbert Dijkhuizen, Anna K. H. Hirsch, Walid A. M. Elgaher, Varsha R. Jumde |
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| Přispěvatelé: | HIPS, Helmholtz-Institut für Pharmazeutische Forschung Saarland, Universitätscampus E8.1 66123 Saarbrücken, Germany., Host-Microbe Interactions, Chemical Biology 2 |
| Jazyk: | angličtina |
| Rok vydání: | 2020 |
| Předmět: |
synthesis
010402 general chemistry 01 natural sciences Biochemistry drug discovery Small Molecule Libraries Structure-Activity Relationship chemistry.chemical_compound Bacterial Proteins Very Important Paper Drug Discovery Dynamic combinatorial chemistry Combinatorial Chemistry Techniques General Pharmacology Toxicology and Pharmaceutics Surface plasmon resonance Pharmacology chemistry.chemical_classification dynamic combinatorial chemistry Bacteria Full Paper biology 010405 organic chemistry Drug discovery Chemistry Organic Chemistry Biofilm Substrate (chemistry) Glycoside glycosides Maltose Surface Plasmon Resonance Full Papers Combinatorial chemistry Anti-Bacterial Agents 0104 chemical sciences Glucosyltransferases biology.protein Molecular Medicine Glucosyltransferase glucosyltransferase Sugars Protein Binding |
| Zdroj: | ChemMedChem International Germany ChemMedChem, 16(1):cmdc.202000222, 113-123. WILEY-V C H VERLAG GMBH Chemmedchem |
| ISSN: | 1860-7179 |
| Popis: | We applied dynamic combinatorial chemistry (DCC) to find novel ligands of the bacterial virulence factor glucosyltransferase (GTF) 180. GTFs are the major producers of extracellular polysaccharides, which are important factors in the initiation and development of cariogenic dental biofilms. Following a structure‐based strategy, we designed a series of 36 glucose‐ and maltose‐based acylhydrazones as substrate mimics. Synthesis of the required mono‐ and disaccharide‐based aldehydes set the stage for DCC experiments. Analysis of the dynamic combinatorial libraries (DCLs) by UPLC‐MS revealed major amplification of four compounds in the presence of GTF180. Moreover, we found that derivatives of the glucose‐acceptor maltose at the C1‐hydroxy group act as glucose‐donors and are cleaved by GTF180. The synthesized hits display medium to low binding affinity (K D values of 0.4–10.0 mm) according to surface plasmon resonance. In addition, they were investigated for inhibitory activity in GTF‐activity assays. The early‐stage DCC study reveals that careful design of DCLs opens up easy access to a broad class of novel compounds that can be developed further as potential inhibitors. Delay decay: Structure‐based design in combination with acylhydrazone‐based dynamic combinatorial chemistry (DCC) afforded inhibitors of glucansucrase (GS), the main virulence factor responsible for dental caries. DCC offered a facile pathway for finding the first hits of GS in the form of glucose‐ and maltose‐based acylhydrazones, mimicking the GS substrate. |
| Databáze: | OpenAIRE |
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