Efficacy of tecovirimat (ST-246) in nonhuman primates infected with variola virus (Smallpox)

Eric M Mucker; Arthur J Goff; Joshua D Shamblin; Douglas W Grosenbach; Inger K Damon; Jason M Mehal; Robert C Holman; Darin Carroll; Nadia Gallardo; Victoria A Olson; Cody J Clemmons; Paul Hudson; Dennis E Hruby

doi:10.1128/AAC.00977-13

Efficacy of tecovirimat (ST-246) in nonhuman primates infected with variola virus (Smallpox)

Antimicrob Agents Chemother. 2013 Dec;57(12):6246-53. doi: 10.1128/AAC.00977-13. Epub 2013 Oct 7.

Authors

Eric M Mucker¹, Arthur J Goff, Joshua D Shamblin, Douglas W Grosenbach, Inger K Damon, Jason M Mehal, Robert C Holman, Darin Carroll, Nadia Gallardo, Victoria A Olson, Cody J Clemmons, Paul Hudson, Dennis E Hruby

Affiliation

¹ United States Army Medical Research Institute of Infectious Diseases (USAMRIID), Fort Detrick, Frederick, Maryland, USA.

Abstract

Naturally occurring smallpox has been eradicated but remains a considerable threat as a biowarfare/bioterrorist weapon (F. Fleck, Bull. World Health Organ. 81:917-918, 2003). While effective, the smallpox vaccine is currently not recommended for routine use in the general public due to safety concerns (http://www.bt.cdc.gov/agent/smallpox/vaccination). Safe and effective countermeasures, particularly those effective after exposure to smallpox, are needed. Currently, SIGA Technologies is developing the small-molecule oral drug, tecovirimat (previously known as ST-246), as a postexposure therapeutic treatment of orthopoxvirus disease, including smallpox. Tecovirimat has been shown to be efficacious in preventing lethal orthopoxviral disease in numerous animal models (G. Yang, D. C. Pevear, M. H. Davies, M. S. Collett, T. Bailey, et al., J. Virol. 79:13139-13149, 2005; D. C. Quenelle, R. M. Buller, S. Parker, K. A. Keith, D. E. Hruby, et al., Antimicrob. Agents Chemother., 51:689-695, 2007; E. Sbrana, R. Jordan, D. E. Hruby, R. I. Mateo, S. Y. Xiao, et al., Am. J. Trop. Med. Hyg. 76:768-773, 2007). Furthermore, in clinical trials thus far, the drug appears to be safe, with a good pharmacokinetic profile. In this study, the efficacy of tecovirimat was evaluated in both a prelesional and postlesional setting in nonhuman primates challenged intravenously with 1 × 10(8) PFU of Variola virus (VARV; the causative agent of smallpox), a model for smallpox disease in humans. Following challenge, 50% of placebo-treated controls succumbed to infection, while all tecovirimat-treated animals survived regardless of whether treatment was started at 2 or 4 days postinfection. In addition, tecovirimat treatment resulted in dramatic reductions in dermal lesion counts, oropharyngeal virus shedding, and viral DNA circulating in the blood. Although clinical disease was evident in tecovirimat-treated animals, it was generally very mild and appeared to resolve earlier than in placebo-treated controls that survived infection. Tecovirimat appears to be an effective smallpox therapeutic in nonhuman primates, suggesting that it is reasonably likely to provide therapeutic benefit in smallpox-infected humans.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Antiviral Agents / administration & dosage
Antiviral Agents / therapeutic use*
Benzamides / administration & dosage
Benzamides / therapeutic use*
Isoindoles / administration & dosage
Isoindoles / therapeutic use*
Macaca
Male
Poxviridae Infections / blood
Poxviridae Infections / drug therapy*
Random Allocation
Treatment Outcome
Variola virus / drug effects*
Variola virus / pathogenicity*

Substances

Antiviral Agents
Benzamides
Isoindoles
tecovirimat