AI Article Synopsis

  • Rift Valley fever virus (RVFV) poses a significant health risk to humans and animals, is transmitted through various means, and currently lacks approved vaccines or treatments.
  • The study evaluates DEF201, an adenovirus-vectored interferon alpha, which provides a potential pre- and post-exposure treatment option in a hamster model of RVFV infection.
  • Administration of DEF201 intranasally showed complete protection from RVFV even when given shortly before exposure, while post-exposure treatment was effective within 6 hours but not later, indicating its promise as a countermeasure against RVFV.

Article Abstract

Rift Valley fever virus (RVFV) causes severe disease in humans and ungulates. The virus can be transmitted by mosquitoes, direct contact with infected tissues or fluids, or aerosol, making it a significant biological threat for which there is no approved vaccine or therapeutic. Herein we describe the evaluation of DEF201, an adenovirus-vectored interferon alpha which addresses the limitations of recombinant interferon alpha protein (cost, short half-life), as a pre- and post-exposure treatment in a lethal hamster RVFV challenge model. DEF201 was delivered intranasally to stimulate mucosal immunity and effectively bypass any pre-existing immunity to the vector. Complete protection against RVFV infection was observed from a single dose of DEF201 administered one or seven days prior to challenge while all control animals succumbed within three days of infection. Efficacy of treatment administered two weeks prior to challenge was limited. Post‑exposure, DEF201 was able to confer significant protection when dosed at 30 min or 6 h, but not at 24 h post-RVFV challenge. Protection was associated with reductions in serum and tissue viral loads. Our findings suggest that DEF201 may be a useful countermeasure against RVFV infection and further demonstrates its broad-spectrum capacity to stimulate single dose protective immunity.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3970158PMC
http://dx.doi.org/10.3390/v6031410DOI Listing

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