Affiliation:
1. Max-Planck Institut für Molekulare Genetik, D-14195 Berlin, Germany1;
2. Hoffmann-LaRoche, CH 4070 Basel, Switzerland2; and
3. IRMA, UniversitéParis VI, 75270 Paris Cedex 06,3 and
4. Department of Physics, Roussel UCLAF, 93230 Romainville,4 France
Abstract
ABSTRACT
Penicillin-resistant isolates of
Streptococcus pneumoniae
generally contain mosaic genes encoding the low-affinity penicillin-binding proteins (PBPs) PBP2x, PBP2b, and PBP1a. We now present evidence that PBP2a and PBP1b also appear to be low-affinity variants and are encoded by distinct alleles in β-lactam-resistant transformants of
S. pneumoniae
obtained with chromosomal donor DNA from a
Streptococcus mitis
isolate. Different lineages of β-lactam-resistant pneumococcal transformants were analyzed, and transformants with low-affinity variants of all high-molecular-mass PBPs, PBP2x, -2a, -2b, -1a, and -1b, were isolated. The MICs of benzylpenicillin, oxacillin, and cefotaxime for these transformants were up to 40, 100, and 50 μg/ml, respectively, close to the MICs for the
S. mitis
donor strain. Recruitment of low-affinity PBPs was accompanied by a decrease in cross-linked muropeptides as revealed by high-performance liquid chromatography of muramidase-digested cell walls, but no qualitative changes in muropeptide chemistry were detected. The growth rates of all transformants were identical to that of the parental
S. pneumoniae
strain. The results stress the potential for the acquisition by
S. pneumoniae
of high-level β-lactam resistance by interspecies gene transfer.
Publisher
American Society for Microbiology
Subject
Molecular Biology,Microbiology
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