Quantitative Microplate-Based Growth Assay for Determination of Antifungal Susceptibility of Histoplasma capsulatum Yeasts

Goughenour, Kristie D.; Balada-Llasat, Joan-Miquel; Rappleye, Chad A.

doi:10.1128/jcm.00795-15

Cited by 45 publications

(45 citation statements)

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“…This confirms the findings of an earlier antifungal susceptibility study of six E. africanus yeast phase isolates (5). There are no well-standardized methods for MIC determination for thermally dimorphic fungi (19); nevertheless, in vitro activities of polyenes (i.e., amphotericin B), azoles, and echinocandins have been established for some of these organisms (20). We used Clinical and Laboratory Standards Institute (CLSI)-approved standards as a guide to yeast and mold phase testing but used a larger inoculum for the mold phase and a prolonged incubation period to facilitate growth and endpoint determinations, in line with previous studies (5,19,(21)(22)(23).…”

Section: Discussionsupporting

confidence: 80%

“…There are no well-standardized methods for MIC determination for thermally dimorphic fungi (19); nevertheless, in vitro activities of polyenes (i.e., amphotericin B), azoles, and echinocandins have been established for some of these organisms (20). We used Clinical and Laboratory Standards Institute (CLSI)-approved standards as a guide to yeast and mold phase testing but used a larger inoculum for the mold phase and a prolonged incubation period to facilitate growth and endpoint determinations, in line with previous studies (5,19,(21)(22)(23). Antifungal susceptibility testing for thermally dimorphic fungi is often limited to the mold phase, results of which may be misleading because the yeast phase is responsible for human disease (20).…”

Section: Discussionmentioning

confidence: 99%

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In Vitro Antifungal Susceptibility of Yeast and Mold Phases of Isolates of Dimorphic Fungal Pathogen Emergomycesafricanus (Formerly Emmonsia sp.) from HIV-Infected South African Patients

et al. 2017

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Disseminated emmonsiosis is an important AIDS-related mycosis in SouthAfrica that is caused by Emergomyces africanus, a newly described and renamed dimorphic fungal pathogen. In vitro antifungal susceptibility data can guide management. Identification of invasive clinical isolates was confirmed phenotypically and by sequencing of the internal transcribed spacer region. Yeast and mold phase MICs of fluconazole, voriconazole, itraconazole, posaconazole, caspofungin, anidulafungin, micafungin, and flucytosine were determined with custom-made frozen broth microdilution (BMD) panels in accordance with Clinical and Laboratory Standards Institute recommendations. MICs of amphotericin B, itraconazole, posaconazole, and voriconazole were determined by Etest. Fifty unique E. africanus isolates were tested. The yeast and mold phase geometric mean (GM) BMD and Etest MICs of itraconazole were 0.01 mg/liter. The voriconazole and posaconazole GM BMD MICs were 0.01 mg/liter for both phases, while the GM Etest MICs were 0.001 and 0.002 mg/liter, respectively. The fluconazole GM BMD MICs were 0.18 mg/liter for both phases. The GM Etest MICs of amphotericin B, for the yeast and mold phases were 0.03 and 0.01 mg/liter. The echinocandins and flucytosine had very limited in vitro activity. Treatment and outcome data were available for 37 patients; in a multivariable model including MIC data, only isolation from blood (odds ratio [OR], 8.6; 95% confidence interval [CI], 1.3 to 54.4; P ϭ 0.02) or bone marrow (OR, 12.1; 95% CI, 1.2 to 120.2; P ϭ 0.03) (versus skin biopsy) was associated with death. In vitro susceptibility data support the management of disseminated emmonsiosis with amphotericin B, followed by itraconazole, voriconazole, or posaconazole. Fluconazole was a relatively less potent agent.

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Section: Discussionsupporting

confidence: 80%

Section: Discussionmentioning

confidence: 99%

In Vitro Antifungal Susceptibility of Yeast and Mold Phases of Isolates of Dimorphic Fungal Pathogen Emergomycesafricanus (Formerly Emmonsia sp.) from HIV-Infected South African Patients

et al. 2017

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“…This is not an insignificant question as the yeast and hyphal forms of the dimorphic fungi can have dramatically different susceptibilities. [62][63][64][65][66][67][68][69] For example, early studies with echinocandins showed antifungal effects on the hyphal form of Histoplasma. 67 However, subsequent tests against the yeast form indicated that caspofungin was anywhere from 20-to 1000-fold less effective.…”

Section: Current Antifungal Optionsmentioning

confidence: 99%

Antifungal therapeutics for dimorphic fungal pathogens

Goughenour

Rappleye

2016

Virulence

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Dimorphic fungi cause several endemic mycoses which range from subclinical respiratory infections to life-threatening systemic disease. Pathogenic-phase cells of Histoplasma, Blastomyces, Paracoccidioides and Coccidioides escape elimination by the innate immune response with control ultimately requiring activation of cell-mediated immunity. Clinical management of disease relies primarily on antifungal compounds; however, dimorphic fungal pathogens create a number of challenges for antifungal drug therapy. In addition to the drug toxicity issues known for current antifungals, barriers to efficient drug treatment of dimorphic fungal infections include natural resistance to the echinocandins, residence of fungal cells within immune cells, the requirement for systemic delivery of drugs, prolonged treatment times, potential for latent infections, and lack of optimized standardized methodology for in vitro testing of drug susceptibilities. This review will highlight recent advances, current therapeutic options, and new compounds on the horizon for treating infections by dimorphic fungal pathogens.

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“…Cell Wall Sensitivity Assays-Yeast cells were grown in 96-well microtiter plates (38) with graded concentrations of antifungal compounds (fluconazole (Glenmark Generics); caspofungin (Merck); and nikkomycin Z (gift from John Galgiani)) and cell wall-destabilizing compounds (Calcofluor White (Sigma); Congo red (MP Biomedicals); SDS; and Uvitex) (39). Growth after 4 days was measured by optical density at 595 nm and compared with the turbidity of wells lacking inhibitors.…”

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confidence: 99%

Eng1 and Exg8 Are the Major α-Glucanases Secreted by the Fungal Pathogen Histoplasma capsulatum

Garfoot

Dearing

VanSchoiack

et al. 2017

Journal of Biological Chemistry

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Edited by Gerald W. HartFungal cell walls contain ␤-glucan polysaccharides that stimulate immune responses when recognized by host immune cells. The fungal pathogen Histoplasma capsulatum minimizes detection of ␤-glucan by host cells through at least two mechanisms: concealment of ␤-glucans beneath ␣-glucans and enzymatic removal of any exposed ␤-glucan polysaccharides by the secreted glucanase Eng1. Histoplasma yeasts also secrete the putative glucanase Exg8, which may serve a similar role as Eng1 in removing exposed ␤-glucans from the yeast cell surface. Here, we characterize the enzymatic specificity of the Eng1 and Exg8 proteins and show that Exg8 is an exo-␤1,3-glucanase and Eng1 is an endo-␤1,3-glucanase. Together, Eng1 and Exg8 account for nearly all of the total secreted glucanase activity of Histoplasma yeasts. Both Eng1 and Exg8 proteins are secreted through a conventional secretion signal and are modified posttranslationally by O-linked glycosylation. Both glucanases have near maximal activity at temperature and pH conditions experienced during infection of host cells, supporting roles in Histoplasma pathogenesis. Exg8 has a higher specific activity than Eng1 for ␤1,3-glucans; yet despite this, Exg8 does not reduce detection of yeasts by the host ␤-glucan receptor Dectin-1. Exg8 is largely dispensable for virulence in vivo, in contrast to Eng1. These results show that Histoplasma yeasts secrete two ␤1,3-glucanases and that Eng1 endoglucanase activity is the predominant factor responsible for removal of exposed cell wall ␤-glucans to minimize host detection of Histoplasma yeasts.

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Quantitative Microplate-Based Growth Assay for Determination of Antifungal Susceptibility of Histoplasma capsulatum Yeasts

Cited by 45 publications

References 44 publications

In Vitro Antifungal Susceptibility of Yeast and Mold Phases of Isolates of Dimorphic Fungal Pathogen Emergomycesafricanus (Formerly Emmonsia sp.) from HIV-Infected South African Patients

In Vitro Antifungal Susceptibility of Yeast and Mold Phases of Isolates of Dimorphic Fungal Pathogen Emergomycesafricanus (Formerly Emmonsia sp.) from HIV-Infected South African Patients

Antifungal therapeutics for dimorphic fungal pathogens

Eng1 and Exg8 Are the Major α-Glucanases Secreted by the Fungal Pathogen Histoplasma capsulatum

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