Abstract

Serine beta-lactamases are the major resistance mechanism to beta-lactam antibiotics, such as penicillin. In the last 20 years, hundreds of mutant beta-lactamases have appeared in response to an ever-growing number of plactams. These enzymes pose a pressing medical problem and a fascinating example of molecular evolution happening as we watch. A goal of this research is to understand the molecular bases of this evolving activity. A second goal is to exploit this information to discover novel beta-lactamase inhibitors, which may escape the current cycle of incremental antibiotic modification followed by rapid resistance response.
The specific aims are: 1. To understand the molecular bases of action of evolved mutant a-lactamases. Outstanding questions include: How do """"""""extended spectrum"""""""" substitutions increase activity against """"""""beta -lactamase-stable"""""""" beta-lactams, such as ceftazidime? Correspondingly, how do """"""""inhibitor resistant"""""""" substitutions confer resistance to inhibitors such as clavulanate? Similar to many resistance enzymes, these substitutions often occur far from the active site-how do they affect activity? Does the increase in activity have a cost? How, for instance, is new activity gained without activity loss against traditional substrates? Correspondingly, do these mutants, which often involve significant re-arrangements of the active site, lose stability? We target mutants of the TEM, CTX-M, and AmpC families, which wide-spread. Characteristic mutants will be cloned, over-expressed, their kinetics measured and their structures determined by x-ray crystallography. Using substrate and transition-state analogs, both apo- and ligand-bound structures will be determined. 2. To discover novel inhibitors of wild-type and mutant a-lactamases. Both novel inhibitors, not resembling beta-lactams, and potent substrate and transition-state analogs, will be designed and tested as agents to reverse a-lactamase-based resistance. Guided by the structural studies from aim 1, the following questions will be explored: Can non-beta-lactams inhibit beta-lactamases potently? Can we imagine an """"""""uber"""""""" inhibitor that will target both WT and the diverse classes of mutant enzymes, or will a more specialist strategy be required? Will novel inhibitors evade the pre-evolved resistance mechanisms that face beta-lactams? Four classes of inhibitors will be synthesized and compared: substrate analogs, transition-state analogs, arylboronic acids, and leads from virtual screening. The Kj values of the new inhibitors and their crystal structures with mutant and WT beta-lactamases will be determined. The antimicrobial synergy of the new inhibitors will be evaluated.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM063815-08
Application #
7470609
Study Section
Synthetic and Biological Chemistry B Study Section (SBCB)
Program Officer
Fabian, Miles
Project Start
2001-08-01
Project End
2010-03-31
Budget Start
2008-08-01
Budget End
2010-03-31
Support Year
8
Fiscal Year
2008
Total Cost
$208,692
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Pharmacology
Type
Schools of Pharmacy
DUNS #
094878337
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Santucci, Matteo; Spyrakis, Francesca; Cross, Simon et al. (2017) Computational and biological profile of boronic acids for the detection of bacterial serine- and metallo-?-lactamases. Sci Rep 7:17716
Tondi, Donatella; Venturelli, Alberto; Bonnet, Richard et al. (2014) Targeting class A and C serine ?-lactamases with a broad-spectrum boronic acid derivative. J Med Chem 57:5449-58
Merski, Matthew; Shoichet, Brian K (2012) Engineering a model protein cavity to catalyze the Kemp elimination. Proc Natl Acad Sci U S A 109:16179-83
Eidam, Oliv; Romagnoli, Chiara; Dalmasso, Guillaume et al. (2012) Fragment-guided design of subnanomolar ýý-lactamase inhibitors active in vivo. Proc Natl Acad Sci U S A 109:17448-53
Minozzi, Manuela; Lattanzi, Gianluca; Benz, Roland et al. (2011) Permeation through the cell membrane of a boron-based ?-lactamase inhibitor. PLoS One 6:e23187
Thomas, Veena L; McReynolds, Andrea C; Shoichet, Brian K (2010) Structural bases for stability-function tradeoffs in antibiotic resistance. J Mol Biol 396:47-59
Tondi, Donatella; Calo, Samuele; Shoichet, Brian K et al. (2010) Structural study of phenyl boronic acid derivatives as AmpC beta-lactamase inhibitors. Bioorg Med Chem Lett 20:3416-9
Jadhav, Ajit; Ferreira, Rafaela S; Klumpp, Carleen et al. (2010) Quantitative analyses of aggregation, autofluorescence, and reactivity artifacts in a screen for inhibitors of a thiol protease. J Med Chem 53:37-51
Eidam, Oliv; Romagnoli, Chiara; Caselli, Emilia et al. (2010) Design, synthesis, crystal structures, and antimicrobial activity of sulfonamide boronic acids as ?-lactamase inhibitors. J Med Chem 53:7852-63
Preti, Lisa; Attanasi, Orazio A; Caselli, Emilia et al. (2010) One-Pot Synthesis of Imidazole-4-Carboxylates by Microwave-Assisted 1,5-Electrocyclization of Azavinyl Azomethine Ylides. European J Org Chem 2010:

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