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. 1987 Oct;329(6139):545-6.
doi: 10.1038/329545a0.

Recovery of immunodeficient mice from a vaccinia virus/IL-2 recombinant infection

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Recovery of immunodeficient mice from a vaccinia virus/IL-2 recombinant infection

I A Ramshaw et al. Nature. 1987 Oct.

Abstract

Vaccinia virus recombinants that express cloned genes encoding antigens of unrelated infectious agents, such as hepatitis B virus and human immunodeficiency virus (HIV), provide a new approach to the development of live vaccines. Although there is evidence that genetically engineered vaccinia viruses have reduced pathogenicity a major obstacle to their use as vaccines is that severe complications can occur after vaccination, especially in immunodeficient individuals. We describe here a recombinant vaccinia virus expressing murine interleukin-2 (IL-2) and show that athymic nude mice infected with the recombinant virus resolve the virus infection rapidly whereas mice infected with control virus develop a progressive vaccinal disease. By incorporating the gene for IL-2 in live virus vaccines it may be possible to prevent the severe complications that arise in recipients with an impaired immune system.

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