The herpes simplex virus type 1 ribonucleotide reductase is required for acute retinal disease

Archives of Virology
C R BrandtD M Albert

Abstract

We have used a herpes simplex virus type 1 (HSV-1) ribonucleotide reductase (RR) null mutant (ICP6 delta) to determine if the HSV-1 RR is required for acute retinal disease. Injection of the ICP6 delta mutant into the vitreous induced mild transient signs of infection (vitreal infiltrate, retinal inflammation, and changes in retinal cytology). In contrast, the parental KOS and a revertant virus (ICP6 delta + 3.1) in which the RR gene had been restored, caused severe retinitis. Injection of media alone also induced mild transient signs of disease. Two months after infection, ICP6 delta injected eyes could not be distinguished from normal eyes. Repeated injection of ICP6 delta (3 times, 2 weeks apart) resulted in vitreal infiltrate near the site of injection but the retina did not appear damaged. The mutant, ICP6 delta, grew to peak titers 1 x 10(3) to 1 x 10(5)-fold lower and cleared faster than KOS or ICP6 delta + 3.1 in the injected eyes suggesting that the reduced virulence was due to reduced ability of the virus to grow. These results show that the viral RR is required for acute retinal disease.

Citations

Jun 23, 2009·Survey of Ophthalmology·Xuyang LiuPaul L Kaufman
Oct 3, 1999·Experimental Eye Research·X LiuP L Kaufman
May 18, 2001·Molecular Therapy : the Journal of the American Society of Gene Therapy·B SpencerC R Brandt
Sep 25, 2007·Toxicon : Official Journal of the International Society on Toxinology·Ou ShaTzi Bun Ng

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