Posaconazole: a potent, extended‐spectrum triazole anti‐fungal for the treatment of serious fungal infections
Identifieur interne : 000108 ( France/Analysis ); précédent : 000107; suivant : 000109Posaconazole: a potent, extended‐spectrum triazole anti‐fungal for the treatment of serious fungal infections
Auteurs : R. Herbrecht [France]Source :
- International Journal of Clinical Practice [ 1368-5031 ] ; 2004-06.
English descriptors
- Teeft :
- Adverse events, Amphotericin, Antifungal, Antimicrob, Antimicrob agents chemother, Antimicrobial, Antimicrobial agents, Aspergillosis, Aspergillus, Bioavailability, Blackwell publishing, Candida, Chemother, Chemotherapy, Clin, Clin microbiol, Clin pract, Clinical microbiology, Clinical success, Clinical trials, Coccidioidomycosis, Courtney, Dos, European congress, Fluconazole, Fumigatus, Fungal, Fungal infections, Fungi, Fusarium, Glabrata, Healthy volunteers, Herbrecht, Immitis, Infectious diseases, Interscience, Interscience conference, Invasive, Invasive aspergillosis, Itraconazole, June, Multiple doses, Murine, Murine model, Pathogen, Pharmacokinetics, Posaconazole, Posaconazole therapy, Pract, Refractory, Sansone, September, September chicago, Success rate, Successful outcomes, Triazole, Untreated controls, Voriconazole, Zygomycetes, Zygomycosis.
Abstract
Posaconazole is a potent, extended‐spectrum, investigational triazole anti‐fungal that is highly active in pre‐clinical in vitro and in vivo models against a wide array of yeasts and moulds, including Aspergillus, Fusarium and Zygomycetes, which are often refractory to polyenes and older azoles. In humans, orally administered posaconazole is absorbed under fed or fasted conditions; however, absorption is significantly improved when it is coadministered with food or liquid nutritional supplements and when the daily dose is divided (into two or four daily doses). Unlike newer azoles, posaconazole is not extensively metabolised by cytochrome P450 (CYP) enzymes and is primarily excreted as parent compound in the faeces. Posaconazole is a CYP3A4 inhibitor, but it does not inhibit the activity of other CYP enzymes. Therefore, in comparison with other azole anti‐fungal drugs, posaconazole may have the potential for fewer drug interactions. The pharmacokinetics of posaconazole are not influenced by age, gender or race. Dose adjustments for renal or hepatic impairment do not appear to be indicated based on results from single‐dose studies. Preliminary efficacy data from clinical trials are promising. As salvage therapy, posaconazole elicited complete or partial responses in 44 to 75% of patients (N = 97) with invasive fungal infections who were intolerant of, or who had disease refractory to, amphotericin B or itraconazole. In an analysis of patients with aspergillosis, a 42% success rate was observed in the posaconazole arm (n = 107) compared with a 26% success rate in the control arm (n = 86). Importantly, Kaplan‐Meier analysis demonstrated a survival benefit in posaconazole‐treated patients. Moreover, posaconazole yielded complete or partial responses in 71% of patients with zygomycosis (N = 24). Posaconazole appears to be well tolerated over long‐term administration (>1 year) and may represent an important addition to the anti‐fungal armamentarium.
Url:
DOI: 10.1111/j.1368-5031.2004.00167.x
Affiliations:
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ISTEX:8B9A64E8A36E4779D3E15A786F52310C29043E73Le document en format XML
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In humans, orally administered posaconazole is absorbed under fed or fasted conditions; however, absorption is significantly improved when it is coadministered with food or liquid nutritional supplements and when the daily dose is divided (into two or four daily doses). Unlike newer azoles, posaconazole is not extensively metabolised by cytochrome P450 (CYP) enzymes and is primarily excreted as parent compound in the faeces. Posaconazole is a CYP3A4 inhibitor, but it does not inhibit the activity of other CYP enzymes. Therefore, in comparison with other azole anti‐fungal drugs, posaconazole may have the potential for fewer drug interactions. The pharmacokinetics of posaconazole are not influenced by age, gender or race. Dose adjustments for renal or hepatic impairment do not appear to be indicated based on results from single‐dose studies. Preliminary efficacy data from clinical trials are promising. As salvage therapy, posaconazole elicited complete or partial responses in 44 to 75% of patients (N = 97) with invasive fungal infections who were intolerant of, or who had disease refractory to, amphotericin B or itraconazole. In an analysis of patients with aspergillosis, a 42% success rate was observed in the posaconazole arm (n = 107) compared with a 26% success rate in the control arm (n = 86). Importantly, Kaplan‐Meier analysis demonstrated a survival benefit in posaconazole‐treated patients. Moreover, posaconazole yielded complete or partial responses in 71% of patients with zygomycosis (N = 24). Posaconazole appears to be well tolerated over long‐term administration (>1 year) and may represent an important addition to the anti‐fungal armamentarium.</div></front></TEI><affiliations><list><country><li>France</li></country><region><li>Alsace (région administrative)</li><li>Grand Est</li></region><settlement><li>Strasbourg</li></settlement></list><tree><country name="France"><region name="Grand Est"><name sortKey="Herbrecht, R" sort="Herbrecht, R" uniqKey="Herbrecht R" first="R." last="Herbrecht">R. Herbrecht</name></region><name sortKey="Herbrecht, R" sort="Herbrecht, R" uniqKey="Herbrecht R" first="R." last="Herbrecht">R. Herbrecht</name></country></tree></affiliations></record>Pour manipuler ce document sous Unix (Dilib)
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