Gentamicin-loaded microspheres for reducing the  intracellular   Brucella abortus load in infected monocytes

doi:10.1093/jac/dkh227

JAC Advance Access published online on April 21, 2004
Journal of Antimicrobial Chemotherapy, doi:10.1093/jac/dkh227
© 2004 by The British Society for Antimicrobial Chemotherapy

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Received November 20, 2003
Revised March 8, 2004
Accepted March 8, 2004

Original article

Gentamicin-loaded microspheres for reducing the intracellular Brucella abortus load in infected monocytes

Sandra Prior ¹, Bruno Gander ², Concepción Lecároz ¹, Juan M. Irache ³, Carlos Gamazo ¹^*

¹ Department of Microbiology, University of Navarra, 31008 Pamplona, Spain;
² Institute of Pharmaceutical Sciences, ETH, 8057 Zürich, Switzerland
³ Department of Pharmacy and Pharmaceutical Technology, University of Navarra, 31008 Pamplona, Spain;

^* To whom correspondence should be addressed. E-mail: cgamazo{at}unav.es.

Abstract

Objectives: The intracellular antibiotic efficiency of gentamicin-loadedmicrospheres in the context of Brucella-infected murine monocyteswas examined in vitro with a view to developing improved therapies forthe treatment of brucellosis.

Methods: Biodegradable microspheresmade of end-group capped and uncapped poly(lactide-co-glycolide)50:50 (PLGA 50:50 and PLGA 50:50H) and containing gentamicinsulphate were used to target Brucella abortus-infected J774monocyte-macrophages. The infected cells were treated with15 µg of free or microencapsulated gentamicin and theefficacy of the treatments was measured after 24 h.

Results:The particle sizes were below 8 µm and in vitro release ofgentamicin from the microspheres followed a continuous (PLGA 50:50H)or a multiphasic (PLGA 50:50) pattern over 50 days. Treatment withgentamicin microencapsulated into the end-group uncapped PLGA 50:50Hmicrospheres, decreased significantly the number of intracellular bacteria(typically by 2 log₁₀) in comparison with untreated infectedcells. Addition of 2% poloxamer 188 to the microsphere dispersionmedium further reduced the infection (3.5 log₁₀). Opsonizationof the particles with non-immune mouse serum had no effecton the antibacterial efficacy of the microspheres. End-group cappedPLGA 50:50 type microspheres containing the antibiotic were lesseffective at reducing intracellular bacteria ( $~$ 1 log₁₀ reduction),although addition of poloxamer 188 to the dispersion mediumagain enhanced their intracellular antibacterial activity.Placebo PLGA 50:50 and PLGA 50:50H microspheres had no bactericidalactivity.

Conclusions: The results indicate that PLGA 50:50-microencapsulatedgentamicin sulphate may be suitable for efficient drug targetingand delivery to reduce intracellular Brucella infections.

Key Words: Keywords: biodegradable microspheres, drug delivery systems, Brucella-infected monocytes

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