Interplay between Two RND Systems Mediating Antimicrobial Resistance in Brucella suis

doi:10.1128/JB.01198-08

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Journal of Bacteriology, April 2009, p. 2530-2540, Vol. 191, No. 8
0021-9193/09/$08.00+0 doi:10.1128/JB.01198-08
Copyright © 2009, American Society for Microbiology. All Rights Reserved.

Interplay between Two RND Systems Mediating Antimicrobial Resistance in Brucella suis

Fernando A. Martin,¹ Diana M. Posadas,¹ Mariela C. Carrica,² Silvio L. Cravero,² David O'Callaghan,³ and Angeles Zorreguieta¹^*

Fundación Instituto Leloir, IIBBA CONICET and FCEyN, Universidad de Buenos Aires, Patricias Argentinas 435, (C1405BWE) Buenos Aires, Argentina,¹ Instituto de Biotecnología, CICVyA, INTA-Castelar, Las Cabañas y Los Reseros s/n (B1712WAA) Castelar, Buenos Aires, Argentina,² Institut National de la Santé et de la Recherche Médicale, ESPRI 26, Université de Montpellier 1, ERA4204, UFR de Médecine, CS 83021, Avenue Kennedy, 30908 NIMES Cedex 02, France³

Received 26 August 2008/ Accepted 23 January 2009

The RND-type efflux pumps are responsible for the multidrugresistance phenotype observed in many clinically relevant species.Also, RND pumps have been implicated in physiological processes,with roles in the virulence mechanisms of several pathogenicbacteria. We have previously shown that the BepC outer membranefactor of Brucella suis is involved in the efflux of diversedrugs, probably as part of a tripartite complex with an innermembrane translocase. In the present work, we characterize twomembrane fusion protein-RND translocases of B. suis encodedby the bepDE and bepFG loci. MIC assays showed that the B. suis ${Delta}$ bepE mutant was more sensitive to deoxycholate (DOC), ethidiumbromide, and crystal violet. Furthermore, multicopy bepDE increasedresistance to DOC and crystal violet and also to other drugs,including ampicillin, norfloxacin, ciprofloxacin, tetracycline,and doxycycline. In contrast to the ${Delta}$ bepE mutant, the resistanceprofile of B. suis remained unaltered when the other RND gene(bepG) was deleted. However, the ${Delta}$ bepE ${Delta}$ bepG double mutant showeda more severe phenotype than the ${Delta}$ bepE mutant, indicating thatBepFG also contributes to drug resistance. An open reading frame(bepR) coding for a putative regulatory protein of the TetRfamily was found upstream of the bepDE locus. BepR stronglyrepressed the activity of the bepDE promoter, but DOC releasedthe repression mediated by BepR. A clear induction of the bepFGpromoter activity was observed only in the BepDE-defective mutant,indicating a regulatory interplay between the two RND effluxpumps. Although only the BepFG-defective mutant showed a moderateattenuation in model cells, the activities of both bepDE andbepFG promoters were induced in the intracellular environmentof HeLa cells. Our results show that B. suis harbors two functionalRND efflux pumps that may contribute to virulence.

* Corresponding author. Mailing address: Fundación Instituto Leloir, IIBBA CONICET and FCEyN, Universidad de Buenos Aires, Patricias Argentinas 435, (C1405BWE) Buenos Aires, Argentina. Phone: 54-11-52387500, ext. 3204. Fax: 54-11-52387501. E-mail: azorreguieta{at}leloir.org.ar

Published ahead of print on 6 February 2009.