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Antimicrobial Agents and Chemotherapy, November 1999, p. 2671-2677, Vol. 43, No. 11
0066-4804/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
Diversity of TEM Mutants in Proteus
mirabilis
R.
Bonnet,1,*
C.
De Champs,1
D.
Sirot,1
C.
Chanal,1
R.
Labia,2 and
J.
Sirot1
Laboratoire de Bactériologie,
Faculté de Médecine, 63001 Clermont-Ferrand
Cedex,1 and UMR 175, CNRS-MNHN,
29000 Quimper,2 France
Received 24 February 1999/Returned for modification 29 June
1999/Accepted 18 August 1999
In a survey of resistance to amoxicillin among clinical isolates of
Proteus mirabilis, 10 TEM-type
-lactamases were
characterized: (i) the well-known penicillinases TEM-1 and TEM-2, the
extended-spectrum
-lactamases (ESBLs) TEM-3 and TEM-24, and the
inhibitor-resistant TEM (IRT) TEM-44 and (ii) five novel enzymes, a
penicillinase TEM-57 similar to TEM-1, an ESBL TEM-66 similar to TEM-3,
and three IRTs, TEM-65, TEM-73, and TEM-74. The penicillinase TEM-57 and the ESBL TEM-66 differed from TEM-1 and TEM-3, respectively, by the
amino acid substitution Gly-92
Asp (nucleotide mutation G-477
A).
This substitution could have accounted for the decrease in pIs (5.2 for
TEM-57 and 6.0 for TEM-66) but did not necessarily affect the intrinsic
activities of these enzymes. The IRT TEM-65 was an IRT-1-like IRT
(Cys-244) related to TEM-2 (Lys-39). The two other IRTs, TEM-73 and
TEM-74, were related to IRT-1 (Cys-244) and IRT-2 (Ser-244),
respectively, and harbored the amino acid substitutions Leu-21
Phe
and Thr-265
Met. In this study, the ESBLs TEM-66, TEM-24, and TEM-3
were encoded by large (170- to 180-kb) conjugative plasmids that
exhibited similar patterns after digestion and hybridization with the
TEM and AAC(6')I probes. The three IRTs TEM-65, TEM-73, and TEM-74 were
encoded by plasmids that ranged in size from 42 to 70 kb but for which
no transfer was obtained. The characterization of five new
plasmid-mediated TEM-type
-lactamases and the first report of TEM-24
in P. mirabilis are evidence of the wide diversity of
-lactamases produced in this species and of its possible role as a
-lactamase-encoding plasmid reservoir.
*
Corresponding author. Mailing address: Faculté de
Médecine, Service de Bactériologie-Virologie, 28, place
Henri Dunant, 63 001 Clermont-Ferrand Cedex, France. Phone: 33 (0)4 73 60 80 18. Fax: 33 (0)4 73 27 74 94. E-mail:
Richard.Bonnet{at}u-clermont1.fr.
Antimicrobial Agents and Chemotherapy, November 1999, p. 2671-2677, Vol. 43, No. 11
0066-4804/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
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