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Authors :
Sofía Mata-Essayag
Sylvia Magaldi
C Hartung de Capriles
Celina Pérez
L. Deibis
G. Verde
Source :
Mycopathologia. 152:135-142
Publication Year :
2000
Publisher :
Springer Science and Business Media LLC, 2000.

Abstract

In the last five years, as HAART has become standard therapy in HIV seropositive or AIDS patients, changes have been noted in the numbers and types of opportunistic fungal infections in these cohorts of patients. Particularly, oropharyngeal candidiasis have become rare in HIV infected patients since the introduction of new anti-HIV drugs of the protease inhibitors type. At the Immunology Institute of the Universidad Central de Venezuela the most frequent protease inhibitors (PIs) used for the treatment of these patients have been: Nelfinavir (ViraceptTM, Roche),Indinavir (Crixivan® Merck),Ritonavir (Norvir®, Abbott),Saquinavir (Fortovase®, Roche).Recently, we observed that recurrent candidiasis was less frequent and no Candidacould be isolated in our patients. A direct relation to the PIs was suspected. In order to assess the “in vitro” antifungal activity of the afore mentioned protease inhibitors on Candida sp., we used both the well diffusion test and the NCCLS broth microdilution test to assay 100 Candida sp. isolates from HIV seropositive or AIDS patients with syntomatic oropharyngeal Candida infection. In general, the data obtained with the well diffusion test were in agreement with those obtained by the broth microdilution test. All 100 isolates were susceptible to Saquinavir and 32 were susceptible to Indinavir using the NCCLS microdilution test,while 97 were susceptible to Saquinavir and 52 to Indinavir by the well diffusion test. From 17 C. albicans resistant to fluconazole, all were susceptible to Saquinavir by the NCCLS micro method and 16 by the well diffusion test. Our results showed anticandidal activity “in vitro” of PIs, mainly Saquinavir.

Details

ISSN :
0301486X
Volume :
152
Database :
OpenAIRE
Journal :
Mycopathologia
Accession number :
edsair.doi...........fd9e87e2b4204d3c4c9c7ebe54aa0dde
Full Text :
https://doi.org/10.1023/a:1013175706355