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Structural and kinetic characterization of a β-lactamase-inhibitor protein

Nature volume 368pages 657–660 (1994)Cite this article

Abstract

THE past decade has seen an alarming worldwide increase in resistance to β-lactam antibiotics among many pathogenic bacteria1, which is due mainly to plasmid- or chromosomally encoded p-lactamases that specifically cleave penicillin and cephalosporins, rendering them inactive. There is therefore a need to develop new strategies in the design of effective inhibitors of β-lactamase. All the small-molecule inhibitors in clinical use are not very effective and are rapidly degraded2,3. Furthermore, newly characterized mutants of the plasmid-mediated β-lactamase TEM-1 are highly resistant to these small-molecule inhibitors, including clavulanic acid and tazobactam4. It has been shown that Streptomyces clavuligerus produces an β-lactamase inhibitory protein (BLIP; MT 17.5 K)5. Here we present data defining BLIP as the most effective known inhibitor of a variety of β-lactamase, with Ki values in the subnanomolar to picomolar range. To identify those features in BLIP that make it such a potent inhibitor, we have determined its molecular structure at 2.1 Å resolution. BLIP is a relatively flat molecule with a unique fold, comprising a tandem repeat of a 76-amino-acid domain. Each domain consists of a helix–loop–helix motif that packs against a four-stranded antiparallel β-sheet (Fig. la). To our knowledge, BLIP is the first example of a protein inhibitor having two similarly folded domains that interact with and inhibit a single target enzyme.

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Author notes

  1. Michael N. G. James: To whom correspondence should be addressed

Authors and Affiliations

  1. Medical Research Council of Canada, Group in Protein Structure and Function, Department of Biochemistry, University of Alberta, Edmonton, Alberta, T6G 2H7, Canada

    Natalie C. J. Strynadka, Kathy Johns, Helen Blanchard & Michael N. G. James

  2. Department of Microbiology, University of Alberta, Edmonton, Alberta, T6G 2E9, Canada

    Susan E. Jensen

  3. F. Hoffmann La Roche Ltd, Department of Preclinical Research Pharmadivision Infectious Diseases, CH-4002, Basel, Switzerland

    Malcolm Page

  4. Laboratory of Enzymology and Centre for Protein Engineering, University of Liége, Sart Tilman, B-4000, Liége, Belgium

    André Matagne & Jean-Marie Frère

Authors
  1. Natalie C. J. Strynadka
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  2. Susan E. Jensen
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  3. Kathy Johns
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  4. Helen Blanchard
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  6. André Matagne
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  7. Jean-Marie Frère
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  8. Michael N. G. James
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Strynadka, N., Jensen, S., Johns, K. et al. Structural and kinetic characterization of a β-lactamase-inhibitor protein. Nature 368, 657–660 (1994). https://doi.org/10.1038/368657a0

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