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Antimicrobial Agents and Chemotherapy, April 1999, p. 868-875, Vol. 43, No. 4
0066-4804/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
Impact of gyrA and parC
Mutations on Quinolone Resistance, Doubling Time, and Supercoiling
Degree of Escherichia coli
Simone
Bagel,
Volker
Hüllen,
Bernd
Wiedemann, and
Peter
Heisig*
Pharmazeutische Mikrobiologie,
Universität Bonn, 53115 Bonn, Germany
Received 22 June 1998/Returned for modification 11 August
1998/Accepted 8 February 1999
Isogenic mutants derived from quinolone-susceptible isolate WT by
introducing gyrA (S83L, D87G) and parC (S80I,
E84K) mutations associated with quinolone resistance were characterized
with respect to quinolone resistance, growth rate, and degree of global
supercoiling. The latter was determined by use of a pair of reporter
plasmids carrying supercoiling-dependent promoters pgyrA
and ptopA, respectively, transcriptionally fused to the
reporter gene bla coding for TEM-1
-lactamase. The
quotient (Qsc) of the
-lactamase specific activity determined for a
mutant carrying either plasmid was taken as a measure of the degree of
global supercoiling. These Qsc data were comparable to results obtained
from the separation of topoisomers of plasmid pBR322 on
chloroquine-containing agarose gels and indicate a reduced degree of
negative supercoiling in resistant mutants relative to the parent, WT.
The S83L mutation in gyrA had the strongest influence on
quinolone resistance while leaving other parameters nearly unaffected.
The gyrA double mutation (S83L plus D87G) had an effect on
quinolone resistance similar to that of a single mutation. Phenotypic
expression of the parC mutation (S80I) was dependent on the
presence of at least one gyrA mutation. Expression of
high-level fluoroquinolone resistance (ciprofloxacin MIC, >4 µg/ml)
required a combination of the gyrA double mutation and one
parC mutation (S80I or E84K). Such mutants showed
considerable alterations of growth rate, global supercoiling, or both.
Introduction of a parC mutation affected neither the
doubling time nor the degree of supercoiling, while the presence of the
gyrA D87G mutation was associated with a significant
reduction in the degree of DNA supercoiling.
*
Corresponding author. Mailing address: Pharmazeutische
Mikrobiologie, Universität Bonn, Meckenheimer Allee 168, 53115 Bonn, Germany. Phone: 49-228-735247. Fax: 49-228-735267. E-mail:
peter.heisig{at}uni-bonn.de.
Antimicrobial Agents and Chemotherapy, April 1999, p. 868-875, Vol. 43, No. 4
0066-4804/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
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