| Literature DB >> 26142222 |
Ahmad Ghavami1, Geneviève Labbé1, Jürgen Brem2, Valerie J Goodfellow1, Laura Marrone1, Carol A Tanner1, Dustin T King3, Melinda Lam1, Natalie C J Strynadka3, Dylan R Pillai4, Stefan Siemann5, James Spencer6, Christopher J Schofield2, Gary I Dmitrienko7.
Abstract
We report on the synthesis of three nitrocefin analogues and their evaluation as substrates for the detection of β-lactamase activity. These compounds are hydrolyzed by all four Ambler classes of β-lactamases. Kinetic parameters were determined with eight different β-lactamases, including VIM-2, NDM-1, KPC-2, and SPM-1. The compounds do not inhibit the growth of clinically important antibiotic-resistant gram-negative bacteria in vitro. These chromogenic compounds have a distinct absorbance spectrum and turn purple when hydrolyzed by β-lactamases. One of these compounds, UW154, is easier to synthesize from commercial starting materials than nitrocefin and should be significantly less expensive to produce.Entities:
Keywords: Antibiotic resistance detection; Chromogenic cephalosporin; Nitrocefin analogues; β-Lactamase
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Year: 2015 PMID: 26142222 DOI: 10.1016/j.ab.2015.06.032
Source DB: PubMed Journal: Anal Biochem ISSN: 0003-2697 Impact factor: 3.365