Structure-based Design and In-Parallel Synthesis of Inhibitors of AmpC b-lactamase

Tondi, D; Powers, R A; Negri, M C; Caselli, M C; Blazquez, J; Costi, M P; Shoichet, B K

Title: Structure-based Design and In-Parallel Synthesis of Inhibitors of AmpC b-lactamase

Journal Article · Mon Mar 08 00:00:00 EST 2010 · Chem. Biol.

OSTI ID:1006356

Tondi, D; Powers, R A; Negri, M C; Caselli, M C; Blazquez, J; Costi, M P; Shoichet, B K ^[1]

Group I {beta}-lactamases are a major cause of antibiotic resistance to {beta}-lactams such as penicillins and cephalosporins. These enzymes are only modestly affected by classic {beta}-lactam-based inhibitors, such as clavulanic acid. Conversely, small arylboronic acids inhibit these enzymes at sub-micromolar concentrations. Structural studies suggest these inhibitors bind to a well-defined cleft in the group I {beta}-lactamase AmpC; this cleft binds the ubiquitous R1 side chain of {beta}-lactams. Intriguingly, much of this cleft is left unoccupied by the small arylboronic acids. To investigate if larger boronic acids might take advantage of this cleft, structure-guided in-parallel synthesis was used to explore new inhibitors of AmpC. Twenty-eight derivatives of the lead compound, 3-aminophenylboronic acid, led to an inhibitor with 80-fold better binding (2; K{sub i} 83 nM). Molecular docking suggested orientations for this compound in the R1 cleft. Based on the docking results, 12 derivatives of 2 were synthesized, leading to inhibitors with K{sub i} values of 60 nM and with improved solubility. Several of these inhibitors reversed the resistance of nosocomial Gram-positive bacteria, though they showed little activity against Gram-negative bacteria. The X-ray crystal structure of compound 2 in complex with AmpC was subsequently determined to 2.1 {angstrom} resolution. The placement of the proximal two-thirds of the inhibitor in the experimental structure corresponds with the docked structure, but a bond rotation leads to a distinctly different placement of the distal part of the inhibitor. In the experimental structure, the inhibitor interacts with conserved residues in the R1 cleft whose role in recognition has not been previously explored. Combining structure-based design with in-parallel synthesis allowed for the rapid exploration of inhibitor functionality in the R1 cleft of AmpC. The resulting inhibitors differ considerably from {beta}-lactams but nevertheless inhibit the enzyme well. The crystal structure of 2 (K{sub i} 83 nM) in complex with AmpC may guide exploration of a highly conserved, largely unexplored cleft, providing a template for further design against AmpC {beta}-lactamase.

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Research Organization:: Argonne National Lab. (ANL), Argonne, IL (United States). Advanced Photon Source (APS)

Sponsoring Organization:: USDOE

OSTI ID:: 1006356

Journal Information:: Chem. Biol., Vol. 8, Issue 2001; ISSN 1074-5521

Country of Publication:: United States

Language:: ENGLISH

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36 MATERIALS SCIENCE
ANTIBIOTICS
BACTERIA
BORONIC ACIDS
CHAINS
CRYSTAL STRUCTURE
DESIGN
ENZYMES
EXPLORATION
LEAD COMPOUNDS
RESIDUES
RESOLUTION
ROTATION
SOLUBILITY
SYNTHESIS

Title: Structure-based Design and In-Parallel Synthesis of Inhibitors of AmpC b-lactamase

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