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Antimicrobial Agents and Chemotherapy, September 2006, p. 3192-3193, Vol. 50, No. 9
0066-4804/06/$08.00+0     doi:10.1128/AAC.00263-06
Copyright © 2006, American Society for Microbiology. All Rights Reserved.

Molecular Characterization of Resistance to Macrolides in Bartonella henselae

Unité des Rickettsies, CNRS UMR 6020, IFR 48, Faculté de Médecine et de Pharmacie, Université de la Méditerranée, 27 Boulevard Jean Moulin, 13385 Marseille Cedex 05, France

Received 2 March 2006/ Returned for modification 11 April 2006/ Accepted 22 June 2006

	ABSTRACT

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We selected in vitro erythromycin-resistant strains of Bartonella henselae. The mutants obtained had point mutations in domain V of 23S rRNA and/or in ribosomal protein L4. One lymph node of a patient with cat-scratch disease had such a mutation in 23S rRNA, suggesting that natural resistant strains may infect humans.

	TEXT

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Bacteria of the genus Bartonella are fastidious, facultative intracellular bacilli, belonging to the alpha-2 subgroup of Proteobacteria. Bartonella henselae is the causative agent of cat-scratch disease (CSD) and is also involved in other clinical situations such as endocarditis, bacillary angiomatosis (BA) and peliosis hepatitis (PH) in immunocompromised patients (1). Interestingly, erythromycin has become the drug of first choice and has been successfully used to treat many patients with BA (8) and PH (14). However, when the treatment duration is less than 15 days, relapses after antibiotic withdrawal are common, and therefore treatment should be given for 3 to 4 months (8). Macrolide compounds inhibit protein synthesis by binding to domains II and V of 23S rRNA (7). The first mechanism of macrolide resistance described was due to posttranscriptional modifications of the 23S rRNA by the adenine-N ⁶-methyltransferase. Modification of the ribosomal target confers cross-resistance to macrolides and remains the most frequent mechanism of resistance. Two other mechanisms of resistance to macrolides have been described: mutations in 23S rRNA gene, L4 and L22 ribosomal proteins (4, 6, 15, 17) and active efflux (16).

For B. henselae, potential mechanisms of resistance to macrolides are not known, and the objective of the present study was to select in vitro erythromycin-resistant (ER) strains to examine the molecular mechanism of resistance. Moreover, the sequences of the macrolide resistance target genes of 15 B. henselae PCR-positive lymph nodes from patients with CSD (18) have been examined to look for possible natural resistance in clinical isolates.

The seven strains of B. henselae used here are described in Table 1. Selection of ER mutants was performed by serial passages of isolates on blood agar plates containing a disk of erythromycin (15 µg) initially placed in the corner of the plate. The plates were incubated at 37°C, and the diameters of growth inhibition (in mm) were measured every 2 weeks. The confluent growth outside the zone of inhibition was harvested with an inoculation loop and subcultured every 2 weeks until the strain became completely resistant. Resistance to erythromycin was defined as an isolate with growth in contact to the disk of erythromycin. The ER and erythromycin-susceptible strains were screened by PCR amplification and DNA sequencing using specific oligonucleotide primers of the entire23S rRNA gene, the L4 and L22 ribosomal proteins described previously (9). The nucleotide sequences obtained were compared by using the CLUSTAL W program supported by the Infobiogen website to look at possible mutations known to be associated with macrolide resistance. The known original sequences of Escherichia coli (K-12 MG1655 [for 23S rRNA gene comparison]) and Streptococcus pneumoniae (TIGR4 [for L4 and L22 genes comparison]) were retrieved from the KEGG Web site and used for sequence alignments. To study a possible heterogeneity of the sequences of the two copies of the domain V of the 23S rRNA gene, PCR products of the ER mutants obtained were cloned in pGEM-T Easy Vector (Promega, Charbonniéres, France), as described by the manufacturer, and 10 clones were sequenced twice.

	ACKNOWLEDGMENTS

 
We thank Paul Newton for help with the manuscript.

	FOOTNOTES

 
* Corresponding author. Mailing address: Unité des Rickettsies, CNRS UMR 6020, IFR 48, Faculté de Médecine et de Pharmacie, Université de la Méditerranée, 27 Blvd. Jean Moulin, 13385 Marseille Cedex 05, France. Phone: (33) 491 38 55 17. Fax: (33) 491 83 03 90. E-mail: jm.rolain{at}medecine.univ-mrs.fr.

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