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Efficacy of CMX001 as a Post Exposure Antiviral in New Zealand White Rabbits Infected with Rabbitpox Virus, a Model for Orthopoxvirus Infections of Humans

CMX001, a lipophilic nucleotide analog formed by covalently linking 3-(hexdecyloxy)propan-1-ol to cidofovir (CDV), is being developed as a treatment for smallpox. In the absence of human cases of smallpox, new treatments must be tested for efficacy in animal models. Previously, we demonstrated the e...

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Autores principales: Rice, Amanda D., Adams, Mathew M., Wallace, Greg, Burrage, Andrew M., Lindsey, Scott F., Smith, Andrew J., Swetnam, Daniele, Manning, Brandi R., Gray, Stacey A., Lampert, Bernhard, Foster, Scott, Lanier, Randall, Robertson, Alice, Painter, George, Moyer, Richard W.
Formato: Texto
Lenguaje:English
Publicado: Molecular Diversity Preservation International (MDPI) 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3046869/
https://www.ncbi.nlm.nih.gov/pubmed/21373379
http://dx.doi.org/10.3390/v3010047
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author Rice, Amanda D.
Adams, Mathew M.
Wallace, Greg
Burrage, Andrew M.
Lindsey, Scott F.
Smith, Andrew J.
Swetnam, Daniele
Manning, Brandi R.
Gray, Stacey A.
Lampert, Bernhard
Foster, Scott
Lanier, Randall
Robertson, Alice
Painter, George
Moyer, Richard W.
author_facet Rice, Amanda D.
Adams, Mathew M.
Wallace, Greg
Burrage, Andrew M.
Lindsey, Scott F.
Smith, Andrew J.
Swetnam, Daniele
Manning, Brandi R.
Gray, Stacey A.
Lampert, Bernhard
Foster, Scott
Lanier, Randall
Robertson, Alice
Painter, George
Moyer, Richard W.
author_sort Rice, Amanda D.
collection PubMed
description CMX001, a lipophilic nucleotide analog formed by covalently linking 3-(hexdecyloxy)propan-1-ol to cidofovir (CDV), is being developed as a treatment for smallpox. In the absence of human cases of smallpox, new treatments must be tested for efficacy in animal models. Previously, we demonstrated the efficacy of CMX001 in protecting New Zealand White rabbits from mortality following intradermal infection with rabbitpox virus as a model for smallpox, monkeypox and for treatment of adverse reactions to smallpox vaccination. Here we extend these studies by exploring different dosing regimens and performing randomized, blinded, placebo-controlled studies. In addition, because rabbitpox virus can be transmitted via naturally generated aerosols (animal to animal transmission), we report on studies to test the efficacy of CMX001 in protecting rabbits from lethal rabbitpox virus disease when infection occurs by animal to animal transmission. In all cases, CMX001 treatment was initiated at the onset of observable lesions in the ears to model the use of CMX001 as a treatment for symptomatic smallpox. The results demonstrate that CMX001 is an effective treatment for symptomatic rabbitpox virus infection. The rabbitpox model has key similarities to human smallpox including an incubation period, generalized systemic disease, the occurrence of lesions which may be used as a trigger for initiating therapy, and natural animal to animal spread, making it an appropriate model.
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spelling pubmed-30468692011-03-01 Efficacy of CMX001 as a Post Exposure Antiviral in New Zealand White Rabbits Infected with Rabbitpox Virus, a Model for Orthopoxvirus Infections of Humans Rice, Amanda D. Adams, Mathew M. Wallace, Greg Burrage, Andrew M. Lindsey, Scott F. Smith, Andrew J. Swetnam, Daniele Manning, Brandi R. Gray, Stacey A. Lampert, Bernhard Foster, Scott Lanier, Randall Robertson, Alice Painter, George Moyer, Richard W. Viruses Review CMX001, a lipophilic nucleotide analog formed by covalently linking 3-(hexdecyloxy)propan-1-ol to cidofovir (CDV), is being developed as a treatment for smallpox. In the absence of human cases of smallpox, new treatments must be tested for efficacy in animal models. Previously, we demonstrated the efficacy of CMX001 in protecting New Zealand White rabbits from mortality following intradermal infection with rabbitpox virus as a model for smallpox, monkeypox and for treatment of adverse reactions to smallpox vaccination. Here we extend these studies by exploring different dosing regimens and performing randomized, blinded, placebo-controlled studies. In addition, because rabbitpox virus can be transmitted via naturally generated aerosols (animal to animal transmission), we report on studies to test the efficacy of CMX001 in protecting rabbits from lethal rabbitpox virus disease when infection occurs by animal to animal transmission. In all cases, CMX001 treatment was initiated at the onset of observable lesions in the ears to model the use of CMX001 as a treatment for symptomatic smallpox. The results demonstrate that CMX001 is an effective treatment for symptomatic rabbitpox virus infection. The rabbitpox model has key similarities to human smallpox including an incubation period, generalized systemic disease, the occurrence of lesions which may be used as a trigger for initiating therapy, and natural animal to animal spread, making it an appropriate model. Molecular Diversity Preservation International (MDPI) 2011-01-24 /pmc/articles/PMC3046869/ /pubmed/21373379 http://dx.doi.org/10.3390/v3010047 Text en © 2011 by the authors; licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution license (http://creativecommons.org/licenses/by/3.0/).
spellingShingle Review
Rice, Amanda D.
Adams, Mathew M.
Wallace, Greg
Burrage, Andrew M.
Lindsey, Scott F.
Smith, Andrew J.
Swetnam, Daniele
Manning, Brandi R.
Gray, Stacey A.
Lampert, Bernhard
Foster, Scott
Lanier, Randall
Robertson, Alice
Painter, George
Moyer, Richard W.
Efficacy of CMX001 as a Post Exposure Antiviral in New Zealand White Rabbits Infected with Rabbitpox Virus, a Model for Orthopoxvirus Infections of Humans
title Efficacy of CMX001 as a Post Exposure Antiviral in New Zealand White Rabbits Infected with Rabbitpox Virus, a Model for Orthopoxvirus Infections of Humans
title_full Efficacy of CMX001 as a Post Exposure Antiviral in New Zealand White Rabbits Infected with Rabbitpox Virus, a Model for Orthopoxvirus Infections of Humans
title_fullStr Efficacy of CMX001 as a Post Exposure Antiviral in New Zealand White Rabbits Infected with Rabbitpox Virus, a Model for Orthopoxvirus Infections of Humans
title_full_unstemmed Efficacy of CMX001 as a Post Exposure Antiviral in New Zealand White Rabbits Infected with Rabbitpox Virus, a Model for Orthopoxvirus Infections of Humans
title_short Efficacy of CMX001 as a Post Exposure Antiviral in New Zealand White Rabbits Infected with Rabbitpox Virus, a Model for Orthopoxvirus Infections of Humans
title_sort efficacy of cmx001 as a post exposure antiviral in new zealand white rabbits infected with rabbitpox virus, a model for orthopoxvirus infections of humans
topic Review
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3046869/
https://www.ncbi.nlm.nih.gov/pubmed/21373379
http://dx.doi.org/10.3390/v3010047
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