Selected article for: "antiviral effect and broad spectrum antiviral effect"
Author: Jara, Miguel O.; Warnken, Zachary N.; Sahakijpijarn, Sawittree; Moon, Chaeho; Maier, Esther Y.; Christensen, Dale J.; Koleng, John J.; Peters, Jay I.; Hackman, Sarah D.; Williams III, Robert O.
Title: Niclosamide Inhalation Powder Made by Thin-Film Freezing: Multi-dose tolerability and exposure in Rats and Pharmacokinetics in Hamsters
  • Cord-id: 7vlqp7xp
  • Document date: 2021_5_12
    • ID: 7vlqp7xp
    Snippet: In this work, we have developed and tested a dry powder form of niclosamide made by thin-film freezing (TFF) and administered it by inhalation to rats and hamsters to gather data about its toxicology and pharmacokinetics. Niclosamide, a poorly water-soluble drug, is an interesting drug candidate because it was approved over 60 years ago for use as an anthelmintic medication, but recent studies demonstrated its potential as a broad-spectrum antiviral with pharmacological effect against SARS-CoV-2
    Document: In this work, we have developed and tested a dry powder form of niclosamide made by thin-film freezing (TFF) and administered it by inhalation to rats and hamsters to gather data about its toxicology and pharmacokinetics. Niclosamide, a poorly water-soluble drug, is an interesting drug candidate because it was approved over 60 years ago for use as an anthelmintic medication, but recent studies demonstrated its potential as a broad-spectrum antiviral with pharmacological effect against SARS-CoV-2 infection. TFF was used to develop a niclosamide inhalation powder composition that exhibited acceptable aerosol performance with a fine particle fraction (FPF) of 86.0% and a mass median aerodynamic diameter (MMAD) and geometric standard deviation (GSD) of 1.11 µm and 2.84, respectively. This formulation not only proved to be safe after an acute three-day, multi-dose tolerability and exposure study in rats as evidenced by histopathology analysis, and also was able to achieve lung concentrations above the required IC90 levels for at least 24 h after a single administration in a Syrian hamster model. To conclude, we successfully developed a niclosamide dry powder inhalation that overcomes niclosamide’s limitation of poor oral bioavailability by targeting the drug directly to the primary site of infection, the lungs.

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