๐ Antiviral effects of antisense morpholino oligomers in murine coronavirus infection models
The recent emergence of novel pathogenic human and animal coronaviruses has highlighted the need for antiviral therapies that are effective against a spectrum of these viruses. We have used several strains of murine hepatitis virus (MHV) in cell culture and in vivo in mouse models to investigate the antiviral characteristics of peptide-conjugated antisense phosphorodiamidate morpholino oligomers (P-PMOs). Ten P-PMOs directed against various target sites in the viral genome were tested in cell culture, and one of these (5TERM), which was complementary to the 5โฒ terminus of the genomic RNA, was effective against six strains of MHV. Further studies were carried out with various arginine-rich peptides conjugated to the 5TERM PMO sequence in order to evaluate efficacy and toxicity and thereby select candidates for in vivo testing. In uninfected mice, prolonged P-PMO treatment did not result in weight loss or detectable histopathologic changes. 5TERM P-PMO treatment reduced viral titers in target organs and protected mice against virus-induced tissue damage. Prophylactic 5TERM P-PMO treatment decreased the amount of weight loss associated with infection under most experimental conditions. Treatment also prolonged survival in two lethal challenge models. In some cases of high-dose viral inoculation followed by delayed treatment, 5TERM P-PMO treatment was not protective and increased morbidity in the treated group, suggesting that P-PMO may cause toxic effects in diseased mice that were not apparent in the uninfected animals. However, the strong antiviral effect observed suggests that with further development, P-PMO may provide an effective therapeutic approach against a broad range of coronavirus infections. Copyright ยฉ 2007, American Society for Microbiology.
keywords
๐ hepatitis virus (437)
๐ weight loss (41)
๐ murine hepatitis (71)
๐ coronavirus infection (270)
๐ viral genome (96)
๐ cell culture (240)
author
๐ค Burrer, Renaud
๐ค Neuman, Benjamin W.
๐ค Ting, Joey P.C.
๐ค Stein, David A.
๐ค Moulton, Hong M.
๐ค Iversen, Patrick L.
๐ค Kuhn, Peter
๐ค Buchmeier, Michael J.
year
โฐ 2007
journal
๐ Journal of Virology
issn
๐ 0022538X
volume
81
number
11
page
5637-5648
citedbycount
56
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