High-Level Expression of Ampc Beta-Lactamase Due to Insertion of Nucleotides between-10 and-35 Promoter Sequences in Escherichia Coli Clinical Isolates: Cases Not Responsive to Extended-Spectrum-Cephalosporin Treatment
Resource
ANTIMICROBIAL AGENTS AND CHEMOTHERAPY v.47 n.7 pp.2138-2144
Journal
ANTIMICROBIAL AGENTS AND CHEMOTHERAPY
Journal Volume
v.47
Journal Issue
n.7
Pages
2138-2144
Date Issued
2003
Date
2003
Author(s)
CHANG, SHAN-CHWEN
Abstract
Two Escherichia coli isolates were recovered from the blood of two cancer patients and were demonstrated to produce high levels of the AmpC beta- lactamase with isoelectric points of >9.0. The hypertranscription of ampC RNA was observed by Northern blot hybridization in both isolates. One isolate ( isolate EC44) had a point mutation (G-->A at position -28) and insertion of thymidine between positions -20 and -19 of the ampC promoter gene (GenBank accession no. AE000487). The single nucleotide insertion of T between positions -19 and- 20 created an optimal distance (17 bp) in the Pribnow box for ampC hyperproduction. The other isolate (isolate EC38) had two point mutations (G-->A at position -28 and C-->T at position +58) and a 2-base (GT) insertion between positions- 14 and -15. Although the insertion of GT between positions- 14 and -15 may create a new promoter next to the original promoter, cloning of the ampC region with truncated nucleotides of the original -35 region of EC38 failed to verify the hypothesis that a new promoter would be created by such a nucleotide insertion. Instead, multiple start sites for ampC transcription at -1, +1, +2, and +3 were observed in an S1 nuclease protection assay. These results suggest that the RNA polymerase is flexible in the selection of a start site in ampC hypertranscription. In conclusion, nucleotide insertions between the -35 and -10 ampC promoter sequences was the mechanism for the hyperproduction of AmpC P-lactamase and resistance to oxyimino-cephalosporins. The failure of the two patients to respond to treatment with oxyimino-cephalosporins highlights the important role of such a resistance mechanism in the clinical setting.
Subjects
FIELD GEL-ELECTROPHORESIS
MOLECULAR-BASIS
RESISTANCE
HYPERPRODUCTION
IDENTIFICATION
MUTATIONS
SDGs
Type
journal article