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Journal of Clinical Microbiology, July 2002, p. 2662-2665, Vol. 40, No. 7
0095-1137/02/$04.00+0     DOI: 10.1128/JCM.40.7.2662-2665.2002
Copyright © 2002, American Society for Microbiology. All Rights Reserved.

Multidrug and Broad-Spectrum Cephalosporin Resistance among Salmonella enterica Serotype Enteritidis Clinical Isolates in Southern Italy

Laura Villa,¹ Caterina Mammina,² Vivi Miriagou,³ Leonidas S. Tzouvelekis,⁴ Panayotis T. Tassios,⁴ Antonino Nastasi,⁵ and Alessandra Carattoli^1*

Laboratory of Bacteriology and Medical Mycology, Istituto Superiore di Sanità, Rome,¹ Centre for Enteric Pathogens of Southern Italy, Department of Hygiene and Microbiology, University of Palermo, Palermo,² Department of Public Health, University of Florence, Florence, Italy,⁵ Laboratory of Bacteriology, Hellenic Pasteur Institute,³ Department of Microbiology, Medical School, University of Athens, Athens, Greece⁴

Received 19 February 2002/ Returned for modification 7 April 2002/ Accepted 21 April 2002

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From 1992 to 1997, only six sporadic isolates of Salmonella enterica serotype Enteritidis from patients with cases of gastroenteritis in southern Italy exhibited resistance to broad-spectrum cephalosporins. Five isolates produced SHV-12, and one isolate encoded a class C ß-lactamase. The bla_SHV-12 gene was located in at least two different self-transferable plasmids, one of which also carried a novel class 1 integron.

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Salmonella enterica serotype Enteritidis is one of the dominant serotypes causing human disease in Europe (6). Most infections caused by serotype Enteritidis and other nontyphoid salmonellae result in self-limiting diarrhea and do not require antimicrobial treatment. However, invasive infections are fairly common in children, for which cases the broad-spectrum cephalosporins are the antibiotics of choice.

During the period 1990 to 1998, the Center for Enteric Pathogens in Palermo, Italy, typed approximately 1,000 salmonella isolates annually, 20% of which belonged to serotype Enteritidis. Of these, approximately 45% were of human origin (13). These had originated primarily from the two epidemiological sentinel hospitals the "G. Di Cristina" pediatric hospital of Palermo and the "Pugliese" hospital of Catanzaro. Phage type PT4 was predominant, represented by 70 to 80% of all isolates, depending on the year. Susceptibility testing, performed according to NCCLS standards by a disk diffusion method (14), showed resistance to broad-spectrum cephalosporins for only six isolates throughout the whole period. Five of these (S76, S78, S79, S86, and S88) belonged to phage type PT4, while the lysis pattern of the sixth (S87) did not conform to a standard type.

Five isolates (S78, S79, S86, S87, and S88) were resistant to ampicillin, ceftazidime, cefotaxime, and aztreonam. They were also positive in the double-disk synergy test (DDST) (10), indicating production of an extended-spectrum ß-lactamase (ESBL). The sixth isolate, S76, was resistant to cefoxitin and amoxicillin-clavulanate but negative in the DDST, thus exhibiting a class C ß-lactamase phenotype (Table 1).

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TABLE 1. Characteristics of six expanded-spectrum cephalosporin-resistant isolates of serotype Enteriditisa

It was possible to transfer ß-lactam resistance from the five DDST-positive isolates to Escherichia coli by conjugation (19), along with all other resistance markers (Table 1).

Isoelectric focusing of ß-lactamases showed that all isolates, except S76, and their respective ceftazidime-resistant transconjugants produced a ß-lactamase that focused at 8.2, suggesting expression of a bla_SHV-like gene (Fig. 1). PCR for bla_SHV (1) and DNA sequencing showed that these isolates carried bla_SHV-12 (EMBL accession no. AY008838). Strain S76 produced a ß-lactamase species with a pI of 9.0 and was positive, by ampC PCR assay and DNA sequencing, for a Citrobacter freundii ampC-derived bla gene (95% homologous, EMBL accession no. D85910).

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FIG. 1. Isoelectric focusing of ß-lactamases, performed in ampholyte-containing polyacrylamide gels (pH range, 3.5 to 9.5), produced by the broad-spectrum cephalosporin-resistant serotype Enteritidis isolates (S76 to S88) and the respective E. coli transconjugants (K78 to K88). ß-Lactamases with known pIs are on the right (lane M).

Plasmids purified from the five E. coli transconjugants and the S76 clinical isolate were digested with EcoRI (Fig. 2). E. coli transconjugants K86 and K88 contained indistinguishable plasmids (ca. 50 kb in size), while transconjugants K78, K79, and K87 contained plasmids of ca. 90 kb with different restriction patterns, though they included some common bands (Fig. 2A).

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FIG. 2. Restriction patterns of plasmids isolated (Concert Purification Midi kit; Life Technologies, Milan, Italy) from five E. coli transconjugant clones and serotype Enteritidis isolate S76. (A) Plasmid fragments were separated by electrophoresis on 0.8% agarose gels and transferred onto positively charged nylon membranes (Boehringer-Mannheim GmbH, Mannheim, Germany). Molecular weight markers (1-kb ladder) are in lane M. (B to D) Southern blot hybridization was performed according to standard protocols (19) with blaSHV-12, C. freundii ampC, and intI1 DNA probes, respectively, labeled with [-32P]dCTP by using the RTS RadPrimer DNA labeling kit (Life Technologies). Primers OS5 and OS6 were used to amplify the blaSHV genes and synthesize the blaSHV-12 DNA probe (1). Primers ampCF (5'-TGGGTTCAGGCCAACATGGATGC-3') and ampCR (5'-TGCCAACATTACGATGCCAAGG-3') were used to amplify the C. freundii ampC-derived gene probe (EMBL accession no. X91840). The intI1 probe was prepared as previously described (21).

Hybridization with the bla_SHV-12 probe demonstrated that this gene was located on the transferred plasmid in each case (Fig. 2B). In spite of two distinct plasmids being present in transconjugant K78 on the one hand and transconjugants K86 and K88 on the other, all three showed an apparently common bla_SHV-12-positive band of approximately 4.0 kb. In contrast, the bla_SHV-12 probe hybridized to distinct EcoRI fragments of the K79 and K87 plasmids. Southern blot hybridization with a C. freundii ampC-specific probe demonstrated that the cephalosporinase gene was also located on a plasmid (Fig. 2C).

The presence of class 1 integrons was investigated for all six clinical isolates by PCR amplification with the 5'CS and 3'CS primer pair (12). Amplicons of a similar size (2.5 kb) were obtained from S78, S79, and S87 and sequenced. Three resistance genes were included as gene cassettes: aacC4, conferring resistance to kanamycin and tobramycin; aadA1, conferring streptomycin-spectinomycin resistance; and catB2, conferring chloramphenicol resistance. This particular structure does not correspond to any of the variable regions of class 1 integrons described so far. The integrons were located on the bla_SHV-12-carrying plasmids, as demonstrated by Southern blot hybridization on plasmid DNA, using an intI1-specific probe (Fig. 2D). The three remaining isolates were negative for the presence of class 1 integrons by both PCR and hybridization with the intI1 probe.

Molecular typing by pulsed-field gel electrophoresis (PFGE) of XbaI-restricted genomic DNA (8) showed that all clinical strains carrying the bla_SHV-12 gene were highly related at the chromosomal level. Their PFGE patterns differed by three to four DNA fragments, classifying them in five subtypes (data not shown). Nevertheless, isolates S78 and S79 had been identified in Sicily 2 years apart and were epidemiologically unrelated. Isolates S86, S87, and S88, however, had been recovered from patients in three gastroenteritis cases that had occurred in Catanzaro, Calabria, during a very brief interval of time. Given the similarity of their PFGE profiles, these isolates may represent a clonal outbreak, though clinical records did not indicate any epidemiological association. The cephalosporinase-producing S76 isolate exhibited a distinct PFGE type.

The present findings constitute further evidence regarding the increasing frequency of isolation of cephalosporin-resistant strains among epidemiologically important Salmonella serotypes. Most other studies so far have focused on S. enterica serotype Typhimurium strains that had acquired plasmids encoding various ESBL types such as TEM, SHV, CTX-M, and PER (20, 22). Recently, serotype Typhimurium strains producing cephalosporinases similar to the chromosomal enzymes of C. freundii have also been reported in the United States (5, 23). However, ß-lactamase-mediated resistance to newer cephalosporins is much more rare in serotypes other than Typhimurium. Class A ESBLs have so far been described for a limited number of Salmonella strains of serotypes Wien, Mbandaka, and antigenic formula 35:c:1,2 in African countries and Senftenberg in India (3, 9, 17, 18). There have also been indications of serotype Enteritidis producing unidentified ESBLs in various countries (2, 4, 7). The present study documents for the first time acquisition of bla genes coding for SHV-12 and a C. freundii-derived class C cephalosporinase by serotype Enteritidis.

In five of the six isolates examined here, resistance was due to the acquisition of plasmids coding for SHV-12. This ESBL resembles SHV-5 and exhibits potent hydrolytic activity against most oxyimino-ß-lactams, including ceftazidime, cefotaxime, and ceftriaxone. There were at least two different types of SHV-12-encoding plasmids, as indicated by the differences in plasmid restriction patterns and the results of hybridization experiments. Therefore, acquisition of the bla_SHV-12 gene could have occurred on more than one separate occasion.

The possibility that serotype Enteritidis acquired "nosocomial" plasmids warrants investigation. The hypothesis of nosocomial acquisition would be in agreement with previous studies indicating that nontyphoid salmonellae producing TEM or SHV ESBLs may have exchanged bla genes with other enterobacteria frequently encountered in hospitals (21, 22). Besides, SHV-12-encoding plasmids have been previously encountered in Klebsiella pneumoniae isolates from hospitals throughout Italy (11, 15). A similar hypothesis could also be formulated for isolate S76, which produced a class C ß-lactamase, since enterobacterial clinical isolates with plasmid-mediated cephalosporinases have been repeatedly reported in European countries and the United States (16, 23).

Production of newer cephalosporin-hydrolyzing ß-lactamases by strains belonging to a predominant phage type of serotype Enteritidis is a disturbing development. Further dissemination of such strains may drastically reduce therapeutic options for severe salmonella infections in children. In addition, salmonella carriage of transmissible plasmids such as those described here may facilitate spread of a variety of resistance determinants to other community-acquired pathogens.

 
We are grateful to Ida Luzzi and Emma Filetici for helpful advice and suggestions. We thank F. Riccobono for DNA sequencing.

This research was supported by grants from the Joint Research and Technology Program between Italy and Greece for 1999-2001 from the Greek General Secretariat for Research and Development of the Ministry of Development and the "Progetto Antibiotico Resistenza 2000" from the Italian Ministry of Health.

 
* Corresponding author. Mailing address: Laboratory of Bacteriology and Medical Mycology, Istituto Superiore di Sanità, Viale Regina Elena 299, 00161 Rome, Italy. Phone: 39-06-4990-3128. Fax: 39-06-4938-7112. E-mail: alecara{at}iss.it.

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Journal of Clinical Microbiology, July 2002, p. 2662-2665, Vol. 40, No. 7
0095-1137/02/$04.00+0     DOI: 10.1128/JCM.40.7.2662-2665.2002
Copyright © 2002, American Society for Microbiology. All Rights Reserved.

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