Previous Article | Next Article 
Antimicrobial Agents and Chemotherapy, June 2000, p. 1585-1587, Vol. 44, No. 6
School of Medicine1 and
Histoplasmosis Reference Laboratory,3
Indiana University; and Veterans' Affairs Medical
Center,7 Indianapolis, Indiana;
University of Alabama at Birmingham, Birmingham,
Alabama2; Infectious Disease
Associates of Kansas City, Kansas City,
Missouri4; University of Michigan and
Veterans Affairs Medical Center, Ann Arbor,
Michigan5; and Janssen Research
Foundation, Beerse, Belgium6
Received 26 October 1999/Returned for modification 4 February
2000/Accepted 19 March 2000
The effects of prolonged itraconazole exposure on the
susceptibility of Candida albicans isolates to itraconazole
and fluconazole have not been well characterized. A recent
placebo-controlled study of long-term itraconazole antifungal
prophylaxis in persons with advanced human immunodeficiency virus
infection afforded the opportunity to address this question. Mucosal
Candida sp. isolates were obtained from subjects who
developed oropharyngeal or esophageal candidiasis, and in vitro
susceptibilities of the last isolate obtained at removal from the study
as a prophylaxis failure were compared in itraconazole and placebo
recipients. More subjects in the placebo group (74 of 146 [51%])
than in the itraconazole group (51 of 149 [34%]) developed mucosal
candidiasis (P = 0.004). A total of 112 isolates were
recovered from 56 of the 74 (76%) subjects with mucosal candidiasis
assigned to the placebo group, compared to 97 isolates from 45 of the
51 (88%) subjects in the itraconazole group. C. albicans
accounted for 98% of isolates in the placebo group and 89% of
isolates in the itraconazole group. The itraconazole MIC at which 50%
of the isolates tested were inhibited (MIC50) for
last-episode isolates from the itraconazole group was 0.125 µg/ml
compared to 0.015 µg/ml for the placebo group subjects,
P = 0.0001. The MIC50 of fluconazole for
the last isolates from the itraconazole group was 1.5 µg/ml compared
to 0.5 µg/ml for the placebo subjects (P = 0.005). A lower proportion of isolates recovered from subjects on itraconazole therapy were classified as susceptible to itraconazole (63%) compared to isolates from the placebo group (96%) (P = 0.001).
Similarly, a lower proportion of C. albicans isolates from
subjects on itraconazole therapy were susceptible to fluconazole (78%)
compared to isolates from the placebo group (96%) (P = 0.01). Also, the proportion of isolates that were not fully
susceptible to itraconazole or fluconazole was greater in patients
assigned to the itraconazole group than the placebo group (itraconazole
susceptibility, 37 and 4%, respectively (P = 0.001);
fluconazole susceptibility, 23 and 4%, respectively
(P = 0.01). In conclusion, long-term itraconazole prophylaxis in patients with AIDS is associated with reduction in
susceptibility to itraconazole and cross-resistance to fluconazole.
0066-4804/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
Does Long-Term Itraconazole Prophylaxis Result in In Vitro Azole
Resistance in Mucosal Candida albicans Isolates from Persons
with Advanced Human Immunodeficiency Virus Infection?
*
Corresponding author. Mailing address: Histoplasmosis
Reference Laboratory, Indiana University School of Medicine, 1001 West 10th St., Indianapolis, IN 46202. Phone: (317) 630-6119. Fax: (317)
630-7522. E-mail: lwheat{at}iupui.edu.
Members of the National Institute of Allergy and Infectious
Diseases Mycoses Study group include C. Flanigan and H. Gutsch (National Institute of Allergy and Infectious Diseases); B. Weissinger, A. Baruch, and A. Dine (Janssen Pharmaceutical); D. Smith and B. Lee
(Infectious Disease Associates of Kansas City); H. Nixon (Indiana
University School of Medicine); D. Bamberger and D. Simpson (University
of Missouri
Kansas City); J. Black, S. Norris, T. Slama, and S. Ryan
(Infectious Disease of Indiana); J. Richardson and J. McKinsey
(Vanderbilt University); D. Lancaster and D. Ray (Methodist Hospital
System); and M. Threlkeld (Infectious Disease Associates of Memphis).
Antimicrobial Agents and Chemotherapy, June 2000, p. 1585-1587, Vol. 44, No. 6
0066-4804/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
This article has been cited by other articles:
-
Datta, K., Jain, N., Sethi, S., Rattan, A., Casadevall, A., Banerjee, U.
(2003). Fluconazole and itraconazole susceptibility of clinical isolates of Cryptococcus neoformans at a tertiary care centre in India: a need for care. J Antimicrob Chemother
52: 683-686
[Abstract] [Full Text] -
Bromuro, C., Torosantucci, A., Chiani, P., Conti, S., Polonelli, L., Cassone, A.
(2002). Interplay between Protective and Inhibitory Antibodies Dictates the Outcome of Experimentally Disseminated Candidiasis in Recipients of a Candida albicans Vaccine. Infect. Immun.
70: 5462-5470
[Abstract] [Full Text] -
PELLETIER, R., LORANGER, L., MARCOTTE, H., DE CAROLIS, E.
(2002). Voriconazole and fluconazole susceptibility of Candida isolates. J Med Microbiol
51: 479-483
[Abstract] [Full Text] -
Arathoon, E. G., Gotuzzo, E., Noriega, L. M., Berman, R. S., DiNubile, M. J., Sable, C. A.
(2002). Randomized, Double-Blind, Multicenter Study of Caspofungin versus Amphotericin B for Treatment of Oropharyngeal and Esophageal Candidiases. Antimicrob. Agents Chemother.
46: 451-457
[Abstract] [Full Text]
Copyright © 2009 by the American Society for Microbiology. For an alternate route to Journals.ASM.org, visit: http://intl-journals.asm.org | More Info»