Treatment of tinea unguium with medium and high doses of ultramicrosize griseofulvin compared with that with itraconazole

Körting, Hans Christian; Schäfer‐Korting, Monika; Zienicke, H.; Georgii, A.; Ollert, Markus

doi:10.1128/aac.37.10.2064

Cited by 61 publications

(20 citation statements)

References 25 publications

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“…This agrees with previous reports, which showed the efficacy in vitro of this allylamine (3,17,18). However, for ITC we obtained MICs that were within the range of expected concentrations in nail with daily oral doses of 100 to 200 mg (4,19). Similar results were obtained by Korting et al (18), who tested numerous isolates of T. rubrum and T. mentagrophytes from patients with tinea unguium, also by a microdilution method.…”

Section: Discussionsupporting

confidence: 82%

Collaborative Evaluation of Optimal Antifungal Susceptibility Testing Conditions for Dermatophytes

et al. 2002

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A multicenter study was conducted to define the most suitable testing conditions for antifungal susceptibility of dermatophytes. Broth microdilution MICs of clotrimazole, itraconazole, and terbinafine were determined in three centers against 60 strains of dermatophytes. The effects of inoculum density (ca. 10 3 and 10 4 CFU/ml), incubation time (3, 7, and 14 days), endpoint criteria for MIC determination (complete [MIC-0] and prominent [MIC-2] growth inhibition), and incubation temperature (28 and 37°C) on intra-and interlaboratory agreement were analyzed. The optimal testing conditions identified were an inoculum of 10 4 CFU/ml, a temperature of incubation of 28°C, an incubation period of 7 days, and MIC-0.Dermatophytes are a group of morphologically and physiologically related molds that cause well-defined infections in vertebrates. The incidence of dermatophytoses has increased over recent years, particularly in immunocompromised patients (29,30,32,33). The choice of the proper treatment is determined by the site and extent of the infection and the species involved, as well as by the efficacy, safety profile, and kinetics of the available drugs. For localized nonextensive lesions, topical therapies with clotrimazole (CLT) are generally used. For tinea unguium, scalp ringworm, extensive infections, or skin lesions with folliculitis, systemic antifungal treatment is necessary (1,4,23,26). Oral drugs such as itraconazole (ITC) and terbinafine (TRB) are the antifungal agents currently most used to treat severe infections (4, 23). Some novel compounds, such as UR-9825, posaconazole, voriconazole, or ravuconazole, also appear to be promising candidates for the treatment of dermatophytosis (2,10,28).In the in vitro method proposed by the National Committee for Clinical Laboratory Standards (NCCLS) for testing molds (25), the dermatophytes were not included. Therefore, it is necessary to develop a reproducible standardized method for these important fungi that would lead to protocols for proper treatment. In recent years, some authors, possibly encouraged by the development of the above-mentioned reference method, have published various articles wherein several species of dermatophytes have been tested (11,27,28,34). In these works, different adaptations or modifications of the NCCLS methods have been assayed, although other techniques have also been used (3,12,15). The results obtained have been clearly contradictory in some aspects, which makes evident the need for standardization and the development of reference methods. Recently, we evaluated the activity of 11 antifungal drugs against an important number of strains of dermatophytes (n ϭ 508) by using a microdilution method (10). In that study the testing conditions adopted were an inoculum size of 10 4 CFU/ml, a temperature and time of incubation of 28°C and 7 days, respectively, and the MIC endpoint determination was 50% growth inhibition for azoles and 100% for the rest. It is unknown whether varying the conditions would have changed the results significantly....

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Section: Discussionsupporting

confidence: 82%

Collaborative Evaluation of Optimal Antifungal Susceptibility Testing Conditions for Dermatophytes

et al. 2002

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“…* Some authors simply failed to present data for all intended outcomes. 15,36,38 The use of line graphs, means without measures of variance, and P values to present clinical cure data hampered the production of a coherent data summary of clinical cure rates. 13 Only Ling et al, 24 Evans and Sigurgeirsson, 17 and Gupta et al 11 presented data in absolute numbers for clinical cures they defined a priori.…”

Section: Clinical Cure Ratesmentioning

confidence: 99%

“…28,29,36 Two studies with small numbers of patients (N = 80) did not detect a difference in patient outcomes with griseofulvin (500 mg/d) and itraconazole (100 mg/d) taken for 24 to 36 weeks: Walsoe et al 29 found that none of their 19 patients were cured with either drug while the 61 patients in the trial by Piepponen et al 28 had cure rates of 30% in the griseofulvin arm and 36% in the itraconazole arm. Korting et al 36 compared 2 different dosages of griseofulvin (660 mg/d and 990 mg/d) with 100-mg/d dosage of itraconazole taken for 18 months but detected no difference in the cure rates (N = 108).…”

Section: Griseofulvin Vs Itraconazolementioning

confidence: 99%

Oral Treatments for Toenail Onychomycosis

Crawford

Young²,

Godfrey³

et al. 2002

Arch Dermatol

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“…Because of this 1/3 less ultramicrosize (than microsize) is needed to get the same effect and results. 19,25,26) The dissolution rate of poorly water-soluble drugs often becomes a rate-limiting step in their absorption from the GI tract. 27,28) Various solubilization methods have been used to increase the drug solubility and dissolution properties, including the use of surfactants, water-soluble carriers, polymeric conjugates, particle size reduction, suitable polymorph, anhydrous or organic solvate forms and solid dispersions.…”

Section: -6)mentioning

confidence: 99%

“…Ultramicrocrystalline form is administered at doses of 330-990 mg/d. 19) Since the bioavailability of poorly water-soluble drugs can be influenced by interactions with food or by the physicochemical conditions in the gastrointestinal (GI) tract, 20) oral preparation of griseofulvin is commonly prescribed to be administered according to a fixed dosing schedule. The oral bioavailability of griseofulvin is highly variable (25 to 70%).…”

Section: -6)mentioning

confidence: 99%

Improving the High Variable Bioavailability of Griseofulvin by SEDDS

Arida

Al-Tabakha

Hamoury

2007

CHEMICAL & PHARMACEUTICAL BULLETIN

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Self-emulsifying drug delivery systems (SEDDS) are mixtures of oils and surfactants, ideally isotropic, and sometimes containing cosolvents, which emulsify spontaneously to produce fine oil-in-water emulsions when introduced into aqueous phase under gentle agitation.1) Recently, SEDDS have been formulated using medium chain triglyceride oils and nonionic surfactants, the latter being less toxic. Upon peroral administration, these systems form fine emulsions (or microemulsions) in gastro-intestinal tract (GIT) with mild agitation provided by gastric mobility.2,3) Potential advantages of these systems include enhanced oral bioavailability enabling reduction in dose, more consistent temporal profiles of drug absorption, selective targeting of drug(s) toward specific absorption window in GIT, and protection of drug(s) from the hostile environment in gut. [4][5][6] The process of self-emulsification proceeds through formation of liquid crystals (LC) and gel phases, the properties of which significantly affect the formation of droplets and interface available for partitioning of drug.5-9) Many workers claim various rational applications of SEDDS for delivering and targeting lipophilic drugs (e.g., WIN 54954, 1) N-4472, 10) idebenone, 11) coenzyme Q10, 12) vitamin E, 13) halofantrine, 14) and cyclosporin A. 15) However, very few reports are available of SEDDS of water insoluble or poorly soluble hydrophobic compounds. Therefore the concept of using griseofulvin in SEDDS was considered for the present study, where the drug is present in solution form.Griseofulvin is an antifungal agent first isolated from a Penicillium spp. in 1939. It is effective after oral ingestion and reaches the skin and hair. It is deposited primarily in keratin precursor cells. Ingestion with a heavy meal and reduction in particle size enhances the absorption of griseofulvin.16) Griseofulvin systematic (IUPAC) name is (2S,6ЈR)-7-chloro-2Ј,4,6-trimethoxy-6Ј-methyl-3H,4ЈH-spiro[1-benzofuran-2,1Ј-cyclohex[2]ene]-3,4Ј-dione (Fig. 1), and its formula is C 17 H 17 ClO 6 with molecular weight 352.766 g/mol. The compound is insoluble in water (8.64 mg/l). It has a logP/hydrophobicity 2.15 (partition system octanol/water), and its pK a /isoelectric point is not available.17) Griseofulvin inhibits fungal mitosis by disrupting the mitotic spindle through interaction with polymerized microtubules. 18)Griseofulvin is administered orally. Its microcrystalline and ultramicrocrystalline forms are available as tablets. The microcrystalline form also comes in a pediatric suspension form. The typical dose of microcrystalline form is 500-1000 mg/d. Ultramicrocrystalline form is administered at doses of 330-990 mg/d. 19) Since the bioavailability of poorly water-soluble drugs can be influenced by interactions with food or by the physicochemical conditions in the gastrointestinal (GI) tract, 20) oral preparation of griseofulvin is commonly prescribed to be administered according to a fixed dosing schedule. The oral bioavailability of griseofulvin is highly varia...

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Treatment of tinea unguium with medium and high doses of ultramicrosize griseofulvin compared with that with itraconazole

Cited by 61 publications

References 25 publications

Collaborative Evaluation of Optimal Antifungal Susceptibility Testing Conditions for Dermatophytes

Collaborative Evaluation of Optimal Antifungal Susceptibility Testing Conditions for Dermatophytes

Oral Treatments for Toenail Onychomycosis

Improving the High Variable Bioavailability of Griseofulvin by SEDDS

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