Literature DB >> 23043117

Fragment-guided design of subnanomolar β-lactamase inhibitors active in vivo.

Oliv Eidam1, Chiara Romagnoli, Guillaume Dalmasso, Sarah Barelier, Emilia Caselli, Richard Bonnet, Brian K Shoichet, Fabio Prati.   

Abstract

Fragment-based design was used to guide derivatization of a lead series of β-lactamase inhibitors that had heretofore resisted optimization for in vivo activity. X-ray structures of fragments overlaid with the lead suggested new, unanticipated functionality and points of attachment. Synthesis of three derivatives improved affinity over 20-fold and improved efficacy in cell culture. Crystal structures were consistent with the fragment-based design, enabling further optimization to a K(i) of 50 pM, a 500-fold improvement that required the synthesis of only six derivatives. One of these, compound 5, was tested in mice. Whereas cefotaxime alone failed to cure mice infected with β-lactamase-expressing Escherichia coli, 65% were cleared of infection when treated with a cefotaxime:5 combination. Fragment complexes offer a path around design hurdles, even for advanced molecules; the series described here may provide leads to overcome β-lactamase-based resistance, a key clinical challenge.

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Year:  2012        PMID: 23043117      PMCID: PMC3491531          DOI: 10.1073/pnas.1208337109

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  37 in total

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5.  Structures of ceftazidime and its transition-state analogue in complex with AmpC beta-lactamase: implications for resistance mutations and inhibitor design.

Authors:  R A Powers; E Caselli; P J Focia; F Prati; B K Shoichet
Journal:  Biochemistry       Date:  2001-08-07       Impact factor: 3.162

Review 6.  The behavior and significance of slow-binding enzyme inhibitors.

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7.  Hydrolysis of third-generation cephalosporins by class C beta-lactamases. Structures of a transition state analog of cefotoxamine in wild-type and extended spectrum enzymes.

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8.  Nanomolar inhibitors of AmpC beta-lactamase.

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9.  Detection of ligand binding hot spots on protein surfaces via fragment-based methods: application to DJ-1 and glucocerebrosidase.

Authors:  Melissa R Landon; Raquel L Lieberman; Quyen Q Hoang; Shulin Ju; Jose M M Caaveiro; Susan D Orwig; Dima Kozakov; Ryan Brenke; Gwo-Yu Chuang; Dmitry Beglov; Sandor Vajda; Gregory A Petsko; Dagmar Ringe
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10.  Substrate specificity of human pancreatic elastase 2.

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  30 in total

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4.  Structure-Based Analysis of Boronic Acids as Inhibitors of Acinetobacter-Derived Cephalosporinase-7, a Unique Class C β-Lactamase.

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Review 6.  Structural approaches to pathway-specific antimicrobial agents.

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7.  Crystal Structures of KPC-2 and SHV-1 β-Lactamases in Complex with the Boronic Acid Transition State Analog S02030.

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8.  Exploring the potential of boronic acids as inhibitors of OXA-24/40 β-lactamase.

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9.  Covalent docking of selected boron-based serine beta-lactamase inhibitors.

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