Author:
Meletiadis Joseph,Al-Saigh Rafal,Velegraki Aristea,Walsh Thomas J.,Roilides Emmanuel,Zerva Loukia
Abstract
ABSTRACTIn conventional ΜΙC tests, fungi are exposed to constant drug concentrations, whereasin vivo, fungi are exposed to changing drug concentrations. Therefore, we developed a newin vitropharmacokinetic/pharmacodynamic model where human plasma pharmacokinetics of standard doses of 1 mg/kg amphotericin B, 4 mg/kg voriconazole, and 1 mg/kg caspofungin were simulated and their pharmacodynamic characteristics were determined against three clinical isolates ofAspergillus fumigatus,Aspergillus flavus, andAspergillus terreuswith identical MICs (1 mg/liter for amphotericin B, 0.5 mg/liter for voriconazole) and minimum effective concentrations (0.5 mg/liter for caspofungin). This new model consists of an internal compartment (a 10-ml dialysis tube made out of a semipermeable cellulose membrane allowing the free diffusion of antifungals but not galactomannan) inoculated withAspergillusconidia and placed inside an external compartment (a 700-ml glass beaker) whose content is diluted after the addition of antifungal drugs by a peristaltic pump at the same rate as the clearance of the antifungal drugs in human plasma. Fungal growth was assessed by galactomannan production. Despite demonstrating the same MICs, amphotericin B completely inhibited (100%)A. fumigatusbut notA. flavusandA. terreus, whose growth was delayed for 7.53 and 22.8 h, respectively. Voriconazole partially inhibitedA. fumigatus(49.5%) and Α.flavus(27.9%) but not Α.terreus; it delayed their growth by 3.99 h (A. fumigatus) and 5.37 h (Α.terreus). Caspofungin did not alter galactomannan production in all of the species butA. terreus. The new model simulated human pharmacokinetics of antifungal drugs and revealed important pharmacodynamic differences in their activity.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Pharmacology (medical),Pharmacology
Cited by
42 articles.
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