Posaconazole Prophylaxis in Experimental Systemic Zygomycosis

Barchiesi, Francesco; Spreghini, Elisabetta; Santinelli, Alfredo; Fothergill, Annette W.; Pisa, Eleonora De; Giannini, Daniele; Rinaldi, Michael G.; Scalise, Giorgio

doi:10.1128/aac.00969-06

Cited by 35 publications

(28 citation statements)

References 12 publications

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“…In an animal infection model, PSC showed poor efficacy against a strain of R. oryzae (4). Similarly, prophylactic administration of PSC to neutropenic mice prolonged survival but did not reduce the tissue burden in a disseminated infection caused by R. oryzae (2). The current study partly confirmed these results.…”

supporting

confidence: 80%

Posaconazole Combined with Amphotericin B, an Effective Therapy for a Murine Disseminated Infection Caused by Rhizopus oryzae

Rodríguez

Serena

Mariné

et al. 2008

Antimicrob Agents Chemother

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In a murine model of disseminated zygomycosis, low doses of amphotericin B (0.3 mg/kg body weight/day) combined with posaconazole (40 mg/kg/day) prolonged survival and reduced tissue burden with respect to that of controls and that of both drugs administered alone. Results were similar to those obtained with amphotericin B given alone at 0.8 mg/kg/day.Zygomycosis is an opportunistic fungal infection that causes a high degree of morbidity and mortality in immunocompromised patients, particularly those with hematologic malignancy or diabetes mellitus. Rhyzopus oryzae infection is the most common cause of zygomycosis in humans (10). Optimal management of zygomycosis has not been defined. Rapid diagnosis, mitigation or reduction of risk factors, administration of antifungal therapy, surgical debridement where possible, and the use of adjunctive therapies all contribute to the successful management of zygomycosis (11). Amphotericin B (AMB) deoxycholate and lipid formulations of AMB are the drugs of choice for treating zygomycoses (10,11,12). Posaconazole (PSC) is safer than AMB and shows good in vitro activity against some zygomycetes (1,14). Clinical data seem to confirm that in two compassionate use trials, outcomes obtained with PSC therapy were similar to those obtained with AMB, supporting the use of this azole in the management of refractory zygomycosis or in cases of patient intolerance to AMB therapy (6, 15). Because animal studies showed limited activity of PSC against R. oryzae infection (2, 4), we hypothesized that the combined use of two drugs with different targets and with proven activities against zygomycetes may act synergistically against R. oryzae infection or, at least, would allow the use of reduced therapeutic doses. Therefore, we evaluated the efficacy of PSC alone and of PSC combined with AMB in a model of disseminated R. oryzae infection in neutropenic mice.Two clinical isolates of R. oryzae, FMR 6485 and FMR 8542, were used. The in vitro antifungal susceptibility of each strain was tested using a reference microdilution method (8), and the in vitro interactions were assessed using a checkerboard method (5, 7). For both of the drugs and their combinations, we used a MIC of 0 as the endpoint criterion.Male OF1 mice weighing 30 g were used. All animal care procedures were supervised and approved by the Universitat Rovira i Virgili animal welfare committee. Animals were immunosuppressed by intraperitoneal administration of a single dose of cyclophosphamide, 200 mg/kg of body weight, plus a single intravenous administration of 5-fluorouracil, 150 mg/kg, 1 day before the infection (3). Mice were injected with 1 ϫ 10 5 CFU in 0.2 ml in the lateral tail vein. Preliminary experiments with both strains (data not shown) showed that this concentration was the optimal dose for killing 100% of the animals within 6 days of infection.AMB (Fungizona) and PSC (Noxafil) were tested. AMB was administered intravenously at 0.3 mg/kg/day or 0.8 mg/kg/day, once daily; PSC was administered orally at 20 mg/kg/day, 40 ...

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supporting

confidence: 80%

Posaconazole Combined with Amphotericin B, an Effective Therapy for a Murine Disseminated Infection Caused by Rhizopus oryzae

Rodríguez

Serena

Mariné

et al. 2008

Antimicrob Agents Chemother

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“…68 A few animal studies have been conducted to explore the in vivo efficacy of posaconazole in screening models of disseminated mucormycosis that used survival and/or fungal tissue burden as end points. [69][70][71][72][73] Posaconazole prolonged the survival and reduced tissue burden in neutropenic mice with disseminated Mucor infection and was as effective as standard AmB at the highest dose level. 69 In non-immunocompromised mice, no beneficial effects were observed against R. oryzae, while partial activity was shown against Lichtheimia corymbifera and dose-dependent activity against Rhizopus microsporus.…”

Section: Posaconazolementioning

confidence: 99%

“…In both of these last two studies, AmB significantly prolonged the survival of mice infected with all isolates. 70,72 In a further neutropenic murine model of disseminated R.oryzae mucormycosis, posaconazole had modest, but significant effects on survival that were statistically inferior to AmB at 0.8 mg/kg/day. 73 Finally, in diabetic ketoacidotic or neutropenic mice with disseminated mucormycosis caused by R. oryzae, posaconazole monotherapy did not improve survival or reduce fungal burden as compared to placebo while L-AmB was effective.…”

Section: Posaconazolementioning

confidence: 99%

Diagnosis and treatment of mucormycosis in patients with hematological malignancies: guidelines from the 3rd European Conference on Infections in Leukemia (ECIL 3)

et al. 2012

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“…Considering the low frequency of infection with this organism and the difficulty in obtaining statistically significant data regarding the efficacies of antifungal agents, animal models have proved very useful for this purpose. Previous animal studies evaluating the efficacy of PSC against zygomycetes have included only one or two strains of R. oryzae (3,4,9,19). In the study described here, we have tested a panel of 50 clinical isolates of R. oryzae and, after determining their in vitro susceptibilities to PSC by different methods, have selected a subset of strains with various degrees of susceptibility to evaluate the efficacy of PSC in a murine model of infection.…”

mentioning

confidence: 99%

Correlation between In Vitro Activity of Posaconazole and In Vivo Efficacy against Rhizopus oryzae Infection in Mice

Rodríguez

Pastor

Sutton

et al. 2010

Antimicrob Agents Chemother

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We have evaluated the in vitro activity of posaconazole (PSC) against 50 clinical strains of Rhizopus oryzae using a broth microdilution method, the Neo-Sensitabs tablet diffusion method, and minimal fungicidal concentration (MFC) determination. In general, PSC showed low MICs against this fungus, and the MICs correlated with the inhibition zone diameters. Most of the MFCs, however, were from 1 to 4 dilutions higher than their corresponding MICs. We then investigated the efficacies of several different doses of PSC in a murine model. All treatments began 24 h after challenge and lasted for 7 days. The drug was administered twice a day to mice infected with three strains that showed intermediate PSC susceptibility (MIC ‫؍‬ 2 g/ml) and three PSC-susceptible strains (MIC ‫؍‬ 0.25 g/ml). A dose of 10 mg/kg of body weight was ineffective, while doses of 20 and 30 mg/kg prolonged the survival of the mice. The 50 strains tested were segregated into two groups on the basis of the in vitro data. For the group with the most strains (85%), the strains had low PSC MICs, mice infected with the strains showed higher rates of survival (30 to 40%), and PSC was able to reduce the fungal load in the kidney and less regularly in the brain. For the second group (15% of the strains), the strains had intermediate PSC MICs, mice infected with the strains had lower survival rates (10 to 20%), and PSC treatment resulted in variable and no reductions in the fungal loads in the kidneys and brains, respectively.Infections caused by some fungi of the order Mucorales are highly invasive and potentially fatal, and they mainly affect patients with diabetes mellitus or hematological malignances (20). In a recent survey of the occurrence of Mucorales in clinical samples in the United States, approximately half of the isolates identified belonged to the species Rhizopus oryzae (2). Treatment of Mucorales infections is based on four critical factors: rapid diagnosis, removal of predisposing factors, surgical debridement, and appropriate antifungal therapy, with liposomal amphotericin B (LAMB) being the drug of choice (21). Although posaconazole (PSC) has been demonstrated to be less effective than LAMB for the treatment of human R. oryzae infections and its use is not recommended as the primary treatment, this drug is considered a reasonable option for patients who are refractory to or intolerant of polyenes (8, 22). PSC has been tested as salvage therapy in several clinical trials, 14 to 37% of the patients showed a complete response (8,22). However, even in such cases the actual role of this drug is difficult to assess, as most of these patients had previously been treated with AMB or their lipid formulations. It is also unknown whether these success rates were related to the patients' immune status and/or other conditions or to the susceptibility of the strains involved in these infections. Furthermore, in clinical trials in which PSC has been evaluated, the fungi involved were not identified to the species level, thereby making it impossible t...

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Posaconazole Prophylaxis in Experimental Systemic Zygomycosis

Cited by 35 publications

References 12 publications

Posaconazole Combined with Amphotericin B, an Effective Therapy for a Murine Disseminated Infection Caused by Rhizopus oryzae

Posaconazole Combined with Amphotericin B, an Effective Therapy for a Murine Disseminated Infection Caused by Rhizopus oryzae

Diagnosis and treatment of mucormycosis in patients with hematological malignancies: guidelines from the 3rd European Conference on Infections in Leukemia (ECIL 3)

Correlation between In Vitro Activity of Posaconazole and In Vivo Efficacy against Rhizopus oryzae Infection in Mice

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