Interferons Regulate the Phenotype of Wild-type and Mutant Herpes Simplex Viruses In Vivo

doi:10.1084/jem.189.4.663

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© The Rockefeller University Press, 0022-1007/1999/2/663/ $5.00
The Journal of Experimental Medicine, Volume 189, Number 4, February 15, 1999 663-672

Articles

Interferons Regulate the Phenotype of Wild-type and Mutant Herpes Simplex Viruses In Vivo

David A. Leib^*^,, Travis E. Harrison^*, Kathleen M. Laslo^*, Michael A. Machalek^*, Nathaniel J. Moorman^*, and Herbert W. Virgin^,^,||

From the ^* Departments of Ophthalmology and Visual Sciences and the Department of Molecular Microbiology, the Center for Immunology, and the ^|| Department of Pathology, Washington University School of Medicine, St. Louis, Missouri 63110

Mechanisms responsible for neuroattenuation of herpes simplexvirus (HSV) have been defined previously by studies of mutantviruses in cultured cells. The hypothesis that null mutationsin host genes can override the attenuated phenotype of nullmutations in certain viral genes was tested. Mutants such asthose in infected cell protein (ICP) 0, thymidine kinase, ribonucleotide reductase, virion host shutoff, and ICP34.5 are reduced intheir capacity to replicate in nondividing cells in cultureand in vivo. The replication of these viruses was examined ineyes and trigeminal ganglia for 1–7 d after corneal inoculationin mice with null mutations (–/–) in interferonreceptors (IFNR) for type I IFNs (IFN- ${alpha}$ /βR), type II IFN(IFN- ${gamma}$ R), and both type I and type II IFNs (IFN- ${alpha}$ /β/ ${gamma}$ R).Viral titers in eyes and ganglia of IFN- ${gamma}$ R^–/– micewere not significantly different from congenic controls. However,in IFN- ${alpha}$ /βR^–/– or IFN- ${alpha}$ /β/ ${gamma}$ R^–/– mice, growth of all mutants, including those with significantlyimpaired growth in cell culture, was enhanced by up to 1,000-foldin eyes and trigeminal ganglia. Blepharitis and clinical signs of infection were evident in IFN- ${alpha}$ /βR^–/– andIFN- ${alpha}$ /β/ ${gamma}$ R^–/– but not control mice for all viruses.Also, IFNs were shown to significantly reduce productive infectionof, and spread from intact, but not scarified, corneas. Particularlystriking was restoration of near-normal trigeminal ganglionreplication and neurovirulence of an ICP34.5 mutant in IFN- ${alpha}$ /βR^–/–mice. These data show that IFNs play a major role in limitingmutant and wild-type HSV replication in the cornea and in thenervous system. In addition, the in vivo target of ICP34.5 maybe host IFN responses. These experiments demonstrate an unsuspectedrole for host factors in defining the phenotypes of some HSVmutants in vivo. The phenotypes of mutant viruses thereforecannot be interpreted based solely upon studies in cell culturebut must be considered carefully in the context of host factorsthat may define the in vivo phenotype.

Key Words: herpes simplex virus mutants • interferons • mice • pathogenesis

Address correspondence to David A. Leib, Department of Ophthalmologyand Visual Sciences, Washington University School of Medicine,Box 8096, 660 South Euclid Ave., St. Louis, MO 63110. Phone:314-362-2689; Fax: 314-362-3638; E-mail: leib{at}am.seer.wustl.edu

¹ Abbreviations used in this paper: ICP, infected cell protein;HSV, herpes simplex virus; PKR, double-stranded RNA-dependentprotein kinase R; rr, ribonucleotide reductase; tk, thymidinekinase; vhs, virion host shutoff.

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