4.7 Article

Oral treatment of cowpox and vaccinia virus infections in mice with ether lipid esters of cidofovir

Journal

ANTIMICROBIAL AGENTS AND CHEMOTHERAPY
Volume 48, Issue 2, Pages 404-412

Publisher

AMER SOC MICROBIOLOGY
DOI: 10.1128/AAC.48.2.404-412.2004

Keywords

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Funding

  1. NEI NIH HHS [EY11832, R01 EY011832] Funding Source: Medline
  2. NIAID NIH HHS [N01AI15439, N01-AI-15439, R37 AI029164, AI29164] Funding Source: Medline

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Four newly synthesized ether lipid esters of cidofovir (CDV), hexadecyloxypropyl-CDV (HDP-CDV), octadecyloxyethyl-CDV (ODE-CDV), oleyloxypropyl-CDV (OLP-CDV), and oleyloxyethyl-CDV (OLE-CDV), were found to have enhanced activities against vaccinia virus (W) and cowpox virus (CV) in vitro compared to those of CDV. The compounds were administered orally and were evaluated for their efficacies against lethal CV or W infections in mice. HDP-CDV, ODE-CDV, and OLE-CDV were effective at preventing mortality from CV infection when treatments were initiated 24 h after viral inoculation, but only HDP-CDV and ODE-CDV maintained efficacy when treatments were initiated as late as 72 It postinfection. Oral pretreatment with HDP-CDV and ODE-CDV were also effective when they were given 5, 3, or 1 day prior to inoculation with CV, even when each compound was administered as a single dose. Both HDP-CDV and ODE-CDV were also effective against W infections when they were administered orally 24 or 48 It after infection. In animals treated with HDP-CDV or ODE-CDV, the titers of both CV and W in the liver, spleen, and kidney were reduced 3 to 7 log(10). In contrast, virus replication in the lungs was not significantly reduced. These data indicate that HDP-CDV or ODE-CDV given orally is as effective as CDV given parenterally for the treatment of experimental CV and W infections and suggest that these compounds may be useful for the treatment of orthopoxvirus infections in humans.

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