Early intervention with high-dose acyclovir treatment during primary herpes simplex virus infection reduces latency and subsequent reactivation in the nervous system in vivo
Nm. Sawtell et al., Early intervention with high-dose acyclovir treatment during primary herpes simplex virus infection reduces latency and subsequent reactivation in the nervous system in vivo, J INFEC DIS, 184(8), 2001, pp. 964-971
There remains a lack of agreement on the effect of antiviral therapy on her
pes simplex virus (HSV) latency and subsequent reactivation. To gain insigh
t into this important issue, a single-cell polymerase chain reaction assay
was used to quantify the effects of high-dose acyclovir on latent infection
in a mouse model. Treatment with 50 mg/kg of acyclovir every 8 h reduced t
he number of latently infected neurons by > 90% when treatment was begun be
fore 24 h after infection and by 80% and 70% when begun at 48 or 72 h after
infection, respectively. The biologic significance of these reductions was
evaluated by using a well-established in vivo reactivation model. The numb
er of animals in which virus reactivated was reduced significantly, even wh
en acyclovir therapy was delayed until 72 h after infection, a time when an
imals had developed lesions. These findings indicate that potent antiviral
therapy during early primary HSV infection can reduce the magnitude of the
latent infection, such that a significant decrease in reactivation is obser
ved.