Activities and Ultrastructural Effects of Antifungal Combinations against Simulated
Candida
Endocardial Vegetations
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Published:2008-07
Issue:7
Volume:52
Page:2367-2376
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ISSN:0066-4804
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Container-title:Antimicrobial Agents and Chemotherapy
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language:en
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Short-container-title:Antimicrob Agents Chemother
Author:
Pai Manjunath P.1, Samples Marie L.1, Mercier Renee-Claude1, Spilde Michael N.2
Affiliation:
1. College of Pharmacy 2. Microprobe/SEM Laboratories of the Institute of Meteorics, University of New Mexico, Albuquerque, New Mexico
Abstract
ABSTRACT
In vitro pharmacodynamic model (PDM) simulation of serum antifungal concentrations may predict the value of combination antifungal regimens against
Candida
sp. endocarditis. We investigated the effects of combinations of flucytosine (5FC), micafungin (Mica), and voriconazole (Vor) against
Candida
-infected human platelet-fibrin clots, used as simulated endocardial vegetations (SEVs). Single clinical bloodstream isolates of
Candida albicans
,
Candida glabrata
,
Candida parapsilosis
, and
Candida tropicalis
were used. All four isolates were susceptible to 5FC, while
C. glabrata
was resistant to Vor and
C. tropicalis
had a paradoxical resistance phenotype to Mica. The SEVs were prepared with an initial inoculum of 1 × 10
6
CFU/g of SEV and added to a PDM, which utilized yeast nitrogen broth-2% glucose and incubation at 35°C and simulated antifungal pharmacokinetic profiles. Fungal densities in the SEVs were determined in quadruplicate over 72 h. Scanning electron microscopy (SEM) was used to evaluate treatment and control SEVs. Vor was the least active single agent against all
Candida
spp. except for
C. parapsilosis
, where it was comparable to Mica. In contrast, 5FC was the most active against all
Candida
spp. except for
C. tropicalis
, where it was comparable to Mica. The combination of 5FC plus Vor was superior to either agent alone against
C. parapsilosis
. The combination of Vor plus Mica was inferior to the use of Mica alone against
C. tropicalis
. The triple combination of 5FC plus Vor plus Mica was no better than single or dual agents against any of the
Candida
spp. The ultrastructural features of infected SEVs were unique for each
Candida
sp., with
C. parapsilosis
in particular manifesting friable biofilm clusters. In general, 5FC and Mica were superior in their rates and extents of fungal burden reduction compared to Vor against
Candida
-infected SEVs. Evaluation of 5FC and Mica in animal models of
Candida
endocarditis is warranted.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Pharmacology (medical),Pharmacology
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