Pharmacokinetic evaluation of UK-49,858, a metabolically stable triazole antifungal drug, in animals and humans

Humphrey, Michael; Jevons, S.; Tarbit, M. H.

doi:10.1128/aac.28.5.648

Cited by 348 publications

(194 citation statements)

References 15 publications

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“…This is in agreement with the observations of other investigators (16,28,32,37,38). Since protein binding is reported to be low for Flu (1,14,17), the effect of serum on its antifungal activity was not tested.…”

Section: Discussionsupporting

confidence: 81%

Effects of amphotericin B and fluconazole on the extracellular and intracellular growth of Candida albicans

Etten

Rhee

Kampen

et al. 1991

Antimicrob Agents Chemother

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The effects of amphotericin B and fluconazole on the extracellular and intracellular growth of Candida albicans were studied. With respect to the extracellular growth of C. albicans, antifungal activity was measured in terms of MICs and minimal fungicidal concentrations as well as by determination of the concentration that effectively killed (>99.9%) C. albicans in the absence or presence (amphotericin B only) of serum. Amphotericin B was highly active in terms of killing, even at an increased inoculum size. In the presence of serum, amphotericin B activity was substantially reduced. For fluconazole, activity was restricted to inhibition of fungal growth, even after the inoculum size was reduced. With respect to the intracellular growth of C. albicans, antifungal activity was measured by using monolayers of murine peritoneal macrophages infected with C. albicans and was measured in terms of inhibition of germ tube formation as well'as effective killing (>99%) of C. albicans. Amphotericin B was highly active against C. albicans. At an increased ratio of infection, amphotericin B activity was slightly reduced. Fluconazole had no antifungal activity. Neither a reduction in the ratio of infection nor exposure of C. albicans to fluconaz'ole prior to macrophage ingestion resulted in activity against intracellular C. albicans by fluconazole. Previous exposure of C. albicans to amphotericin B resulted in increased intracellular activity of amphotericin B. The. intracellular antifungal activity of the combination of fluconazole with amphotericin B was les than that of amphotericin B alone. Amphotericin B showed fungicidal activity against C. albicans growing both extracellularly and intracellularly, whereas fluconazole inhibited growth only of extracellular C. albicans. A slight antagonistic effect between fluconazole and aiflphotericin B was found with respect to intracellular as well as extracellular C. albicans.Deep-seated candidal infections are an important cause of morbidity and mortality in immunocompromised patients (15,21,22). The current drug of choice for most systemic mycoses is still amphotericin B (AmB), but its use is restricted by a variety of toxic side effects (6,13,15,21,22). Consequently, there is a need for effective and less toxic drugs for the treatment of patients with these infections. One of these antifungal agents is the triazole fluconazole (Flu) (4,10,14,33,34,41). In vivo experimental studies suggested that Flu is active against disseminated candidiasis (8,9,29,31,32,35,37). Recently, the antifungal efficacy of Flu was demonstrated in persistently granulocytopenic rabbits when it was used for prevention or early treatment (39,40). Little is still known, however, on the role of Flu in the treatment of systemic candidiasis in immunocompromised patients. Since the host defense mechanisms in these patients are severely impaired, the intrinsic antifungal activity of the antifungal agent is of great importance for effective treatment. Unfortunately, standardized in vitro methods for assessment of ...

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Section: Discussionsupporting

confidence: 81%

Effects of amphotericin B and fluconazole on the extracellular and intracellular growth of Candida albicans

Etten

Rhee

Kampen

et al. 1991

Antimicrob Agents Chemother

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“…formulations, the oral bioavailability of fluconazole exceeds 90%, 39 and is unaffected by gastric pH, 40 food intake or gastrointestinal disease. 41 It is hydrophilic with minimal protein binding and therefore achieves good tissue penetration into cerebrospinal fluid, saliva, sputum, vagina, skin 41 and brain tissue.…”

Section: Triazole Antifungalsmentioning

confidence: 99%

Has the era of individualised medicine arrived for antifungals? A review of antifungal pharmacogenomics

Ashbee

Gilleece

2011

Bone Marrow Transplant

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“…The washout times after each treatment were >14 days. In this study, we selected 14 days as the washout period because of the half-life (t 1/2 ) of the drugs and on the basis of the results of other studies in which the washout period ranged from 7 to 14 days [2,7,14,29].…”

Section: Methodsmentioning

confidence: 99%

“…In human liver transplant patients, antifungal prophylaxis with fluconazole (Fcz) significantly reduces the incidence of invasive fungal infections [25]. Fcz penetrates the blood-brain, blood-prostate and blood-ocular barriers, and high concentrations are found in cerebrospinal fluid, urine and ocular fluids [14,31]. Fcz shows efficacy against aspergillosis, candidiasis, coccidioidomycosis, cryptococcosis and histoplasmosis in animal models [10,13,26].…”

mentioning

confidence: 99%

Effect of Multiple Oral Dosing of Fluconazole on the Pharmacokinetics of Cyclosporine in Healthy Beagles

Katayama

Igarashi

Tani

et al. 2008

The Journal of Veterinary Medical Science

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ABSTRACT. Fluconazole (Fcz) is successfully used in human organ transplant patients as an antifungal therapy. However, Fcz can increase the cyclosporine (CsA) trough level and lead to CsA nephrotoxicity. In canine renal transplantation, CsA has been used as a major immunosuppressant, and it is important to control its trough level. However, the interaction of Fcz with CsA has not yet been reported in dogs. In this study, the effect of Fcz treatment on the pharmacokinetics of CsA in four healthy beagles was investigated using a fourperiod crossover design. The treatments included CsA alone (A), CsA + multiple-dose Fcz 50 mg (B), CsA + multiple-dose Fcz 25 mg (C) and CsA + single-dose Fcz 50 mg (D). Blood CsA concentrations were measured at 0.5, 1, 2, 4, 6, 8, 10, 12 and 24 hr after CsA administration. The AUC 0-12 and C max values for treatment B were significantly higher than those for the other treatments. In particular, the AUC 0-12 of treatment B was about two times higher than that of treatment A. Fcz administration did not significantly prolong the half-life or mean residence time of CsA. The results of our study show that administration of multiple therapeutic doses of Fcz can significantly increase the CsA blood concentration, which might partially depend upon the Fcz blood concentration. When Fcz is used in CsA-based canine renal transplantation, it may be necessary to adjust the CsA trough level by decreasing the dose.

show abstract

Pharmacokinetic evaluation of UK-49,858, a metabolically stable triazole antifungal drug, in animals and humans

Cited by 348 publications

References 15 publications

Effects of amphotericin B and fluconazole on the extracellular and intracellular growth of Candida albicans

Effects of amphotericin B and fluconazole on the extracellular and intracellular growth of Candida albicans

Has the era of individualised medicine arrived for antifungals? A review of antifungal pharmacogenomics

Effect of Multiple Oral Dosing of Fluconazole on the Pharmacokinetics of Cyclosporine in Healthy Beagles

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