Kitces E N, Payne W J, Morahan P S, Tew J G, Murray B K
IARC Sci Publ (1971). 1978(24 Pt 2):1027-32.
A mouse model system was developed for studying the pathogenesis of oral infection with herpes simplex virus type 1 and the protection offered by prior immunization with a nucleic acid-free vaccine. Of non-immunized mice, 95-100% developed ulcerative lesions 3-5 days following application of virus to abraded oral epithelial surfaces. Infection of the ipsilateral sensory (trigeminal) ganglion and the cerebellum occurred by day 2 and sequentially progressed to the contralateral ganglion by day 4 and to the cerebrum by day 5. Prior immunization of mice with an inactivated virus vaccine, and most importantly, with a vaccine free of nucleic acid, protected mice from subsequent oral virus infection. Protection was demonstrated by: (i) reduction in the incidence and severity of primary oral lesions; (ii) a decrease in the number of mice with acute ganglionic infection or dying of encephalitis; and (iii) a reduction in the incidence of latent trigeminal ganglionic infection.
开发了一种小鼠模型系统,用于研究1型单纯疱疹病毒口腔感染的发病机制以及无核酸疫苗预先免疫所提供的保护作用。在未免疫的小鼠中,95%-100%在将病毒应用于磨损的口腔上皮表面后3-5天出现溃疡性病变。同侧感觉(三叉神经)节和小脑在第2天发生感染,并在第4天依次发展至对侧神经节,在第5天发展至大脑。用灭活病毒疫苗,最重要的是用无核酸疫苗预先免疫小鼠,可保护小鼠免受随后的口腔病毒感染。保护作用表现为:(i)原发性口腔病变的发生率和严重程度降低;(ii)急性神经节感染或死于脑炎的小鼠数量减少;(iii)潜伏性三叉神经节感染的发生率降低。