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Multicenter, randomized study of the efficacy and safety of intravenous iclaprim in complicated skin and skin structure infections

  • D. Krievins
  • , R. Brandt
  • , S. Hawser
  • , P. Hadvary
  • , K. Islam*
  • *Šī darba korespondējošais autors
  • Paula Stradina Clinical University Hospital
  • Arpida Ltd
  • International Health Management Associates, Inc.
  • Ki Consulting AG

Zinātniskās darbības rezultāts: Devums žurnālamZinātniskais raksts (žurnālā)koleģiāli recenzēts

34 Atsauces (Scopus)

Kopsavilkums

Iclaprim is a novel antibacterial agent that is currently in development for the treatment of complicated skin and skin structure infections (cSSSI). Iclaprim specifically and selectively inhibits bacterial dihydrofolate reductase, a critical enzyme in the bacterial folate pathway, and exhibits an extended spectrum of activity against various resistant pathogens, including methicillin (meticillin)-resistant Staphylococcus aureus (MRSA). The objective of this randomized, double-blind phase II study was to compare the efficacy and safety of iclaprim to those of vancomycin in patients with cSSSI. Patients were randomized to receive 0.8 mg iclaprim/kg of body weight, 1.6 mg/kg iclaprim, or 1 g vancomycin twice a day for 10 days. Clinical cure rates for the 0.8- and 1.6-mg/kg-iclaprim treatment groups were comparable to that for the vancomycin treatment group (26/28 patients [92.9%], 28/31 patients [90.3%], and 26/28 patients [92.9%], respectively). Iclaprim also showed high microbiological eradication rates. Iclaprim exhibited an eradication rate of 80% and 72% versus 59% observed with vancomycin for S. aureus, the pathogen most frequently isolated at baseline. Five MRSA cases were observed, four in the 0.8-mg/kg-iclaprim arm and one in the vancomycin arm, and all were both clinically and microbiologically cured. Iclaprim exhibited a safety profile similar to that of vancomycin, an established drug for the treatment of cSSSI. Results from this study indicate that iclaprim is a promising new therapy for the treatment of cSSSI, in particular those caused by S. aureus, including MRSA.

OriģinālvalodaAngļu
Lapas (no-līdz)2834-2840
Lapu skaits7
ŽurnālsAntimicrobial Agents and Chemotherapy
Sējums53
Izdevuma numurs7
DOIs
Publikācijas statussPublicēts - jūl. 2009
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