Strategic Design of an Effective beta-Lactamase Inhibitor

Pattanaik, P; Bethel, C; Hujer, A; Hujer, K; Distler, A; Taracila, M; Anderson, V; Fritsche, T; Jones, R

doi:10.1074/jbc.M806833200

Title: Strategic Design of an Effective beta-Lactamase Inhibitor

Journal Article · Thu Jan 01 00:00:00 EST 2009 · Journal of Biological Chemistry

DOI:https://doi.org/10.1074/jbc.M806833200· OSTI ID:980478

Pattanaik, P; Bethel, C; Hujer, A; Hujer, K; Distler, A; Taracila, M; Anderson, V; Fritsche, T; Jones, R

In an effort to devise strategies for overcoming bacterial beta-lactamases, we studied LN-1-255, a 6-alkylidene-2'-substituted penicillin sulfone inhibitor. By possessing a catecholic functionality that resembles a natural bacterial siderophore, LN-1-255 is unique among beta-lactamase inhibitors. LN-1-255 combined with piperacillin was more potent against Escherichia coli DH10B strains bearing bla(SHV) extended-spectrum and inhibitor-resistant beta-lactamases than an equivalent amount of tazobactam and piperacillin. In addition, LN-1-255 significantly enhanced the activity of ceftazidime and cefpirome against extended-spectrum cephalosporin and Sme-1 containing carbapenem-resistant clinical strains. LN-1-255 inhibited SHV-1 and SHV-2 beta-lactamases with nm affinity (K(I) = 110 +/- 10 and 100 +/- 10 nm, respectively). When LN-1-255 inactivated SHV beta-lactamases, a single intermediate was detected by mass spectrometry. The crystal structure of LN-1-255 in complex with SHV-1 was determined at 1.55A resolution. Interestingly, this novel inhibitor forms a bicyclic aromatic intermediate with its carbonyl oxygen pointing out of the oxyanion hole and forming hydrogen bonds with Lys-234 and Ser-130 in the active site. Electron density for the 'tail' of LN-1-255 is less ordered and modeled in two conformations. Both conformations have the LN-1-255 carboxyl group interacting with Arg-244, yet the remaining tails of the two conformations diverge. The observed presence of the bicyclic aromatic intermediate with its carbonyl oxygen positioned outside of the oxyanion hole provides a rationale for the stability of this inhibitory intermediate. The 2'-substituted penicillin sulfone, LN-1-255, is proving to be an important lead compound for novel beta-lactamase inhibitor design.

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Research Organization:: Brookhaven National Lab. (BNL), Upton, NY (United States). National Synchrotron Light Source

Sponsoring Organization:: Doe - Office Of Science

DOE Contract Number:: DE-AC02-98CH10886

OSTI ID:: 980478

Report Number(s):: BNL-93396-2010-JA; JBCHA3; TRN: US201015%%1863

Journal Information:: Journal of Biological Chemistry, Vol. 284; ISSN 0021-9258

Country of Publication:: United States

Language:: English

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08 HYDROGEN
36 MATERIALS SCIENCE
AFFINITY
AROMATICS
CARBONYLS
CRYSTAL STRUCTURE
DESIGN
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ESCHERICHIA COLI
HOLES
HYDROGEN
LEAD COMPOUNDS
MASS SPECTROSCOPY
OXYGEN
PENICILLIN
RESOLUTION
STABILITY
STRAINS
SULFONES
national synchrotron light source

Title: Strategic Design of an Effective beta-Lactamase Inhibitor

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