In Vitro Activities of Daptomycin, Arbekacin, Vancomycin, and Gentamicin Alone and/or in Combination against Glycopeptide Intermediate-Resistant Staphylococcus aureus in an Infection Model

doi:10.1128/AAC.44.7.1925-1929.2000

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Antimicrobial Agents and Chemotherapy, July 2000, p. 1925-1929, Vol. 44, No. 7
0066-4804/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

In Vitro Activities of Daptomycin, Arbekacin, Vancomycin, and Gentamicin Alone and/or in Combination against Glycopeptide Intermediate-Resistant Staphylococcus aureus in an Infection Model

Ronda L. Akins¹^,² and Michael J. Rybak¹^,²^,³^,^*

The Anti-Infective Research Laboratory, Department of Pharmacy Services, Detroit Receiving Hospital and University Health Center,¹ and College of Pharmacy and Allied Health Professions² and School of Medicine,³ Wayne State University, Detroit, Michigan 48201

Received 20 December 1999/Returned for modification 15 February 2000/Accepted 26 April 2000

Daptomycin, a lipopeptide antibiotic, has broad activity against gram-positive organisms, similar to vancomycin; however,its mechanism of action differs, resulting in interference withcell membrane transport and a more rapid bactericidal activity.In light of increasing need for alternative treatments againstintermediate-resistant Staphylococcus aureus, there is revitalizedinterest in this antibiotic. We, therefore, evaluated the activityof daptomycin alone or in combination in an in vitro infectionmodel against two glycopeptide intermediate-resistant S. aureus(GISA) isolates. Newly designed regimens of daptomycin at 4 and6 mg/kg of body weight every 24 h (q24h) were compared to theprevious regimen of 3 mg/kg q12h. Daptomycin MICs and minimalbactericidal concentrations (MBCs) (MIC/MBC) for Mu-50, HIP5836(992), and MRSA-67 were 0.5/1.0, 0.5/1.0, and 0.125/0.5 µg/ml,respectively. MICs and MBCs of arbekacin for the three strainswere 2.0/8.0, 0.125/0.5, and 0.125/0.25 µg/ml, respectively. Vancomycinand gentamicin MICs and MBCs for the three strains were 8.0/8.0,8.0/8.0, and 0.5/1.0 µg/ml and 128/128, 0.5/1.0, and 0.25/0.5µg/ml, respectively. Our experience with daptomycin in an in vitroinfection model has shown significant kill against the two GISAstrains (Mu-50 and 992) (P < 0.03). We also noted that kill wasrelated to a total dose effect for 992, in which simulated daptomycinin vivo dosages of 6 mg/kg q24h and 3 mg/kg q12h produced similarkill and 4 mg/kg q24h resulted in significant regrowth (P $<=$ 0.05).Combination therapy with arbekacin resulted in synergistic activityagainst Mu-50. Daptomycin area under the concentration-time curve/MICand C_max/MIC ranges for GISA isolates were 80 to 116 and 6 to12, respectively, and ranges for MRSA-67 were 320 to 461 and 24to 48, respectively, and appeared to have an association withkill (i.e., decreased CFU/milliliter) at 24 and 48 h. Therefore,these experiments suggest that daptomycin alone or in combinationcould provide an alternative for the treatment ofGISA.

^* Corresponding author. Mailing address: The Anti-Infective Research Laboratory, Department of Pharmacy Services (1B), DetroitReceiving Hospital and University Health Center, 4201 St. AntoineBlvd., Detroit, MI 48201. Phone: (313) 745-4554. Fax: (313) 993-2522.E-mail: mrybak{at}dmc.org.

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