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γ干扰素在眼部的异位表达可保护转基因小鼠免受单纯疱疹病毒1型的眼内感染。

Ectopic expression of gamma interferon in the eye protects transgenic mice from intraocular herpes simplex virus type 1 infections.

作者信息

Geiger K, Howes E L, Sarvetnick N

机构信息

Department of Neuropharmacology, Scripps Research Institute, La Jolla, California 92037.

出版信息

J Virol. 1994 Sep;68(9):5556-67. doi: 10.1128/JVI.68.9.5556-5567.1994.

Abstract

Transgenic (rho gamma) mice provide a model for studying the influence of gamma interferon (IFN-gamma) produced in the eye on ocular and cerebral viral infection. To establish this model, we injected BALB/c- and C57BL/6-derived transgenic and nontransgenic mice of different ages intravitreally with herpes simplex virus type 1 (HSV-1) strain F. Eye and brain tissues of these mice were assessed for pathological and immunocytochemical changes. HSV-1 infection induced severe retinitis of the injected eyes and infection of the brain in all mice. In transgenic mice inoculated with HSV-1, the left, nontreated eyes were protected from retinitis, whereas nontransgenic mice developed bilateral retinitis. Additional intravitreal injection of IFN-gamma with the virus protected the noninoculated eyes of nontransgenic mice. Three-week-old nontransgenic mice died from HSV-1 infection, whereas transgenic mice of the same age and nontransgenic mice intravitreally treated with IFN-gamma survived. Ocular IFN-gamma production increased the extent of inflammation in transgenic mice but did not have a significant influence on the growth of HSV-1 until day 3 after inoculation and did not influence the neuroinvasion of this virus. Thus, the effects of IFN-gamma were not caused by an early block of viral replication. Possible mechanisms of IFN-gamma action include activation of the immune response, alteration of the properties of the virus, and direct protection of neurons.

摘要

转基因(rhoγ)小鼠为研究眼部产生的γ干扰素(IFN-γ)对眼部和脑部病毒感染的影响提供了一个模型。为建立该模型,我们将不同年龄的BALB/c和C57BL/6来源的转基因和非转基因小鼠玻璃体内注射单纯疱疹病毒1型(HSV-1)F株。对这些小鼠的眼和脑组织进行病理和免疫细胞化学变化评估。HSV-1感染在所有小鼠中均诱发了注射眼的严重视网膜炎和脑部感染。在接种HSV-1的转基因小鼠中,未处理的左眼免受视网膜炎影响,而非转基因小鼠则发展为双侧视网膜炎。与病毒一起额外玻璃体内注射IFN-γ可保护非转基因小鼠未接种的眼睛。3周龄的非转基因小鼠死于HSV-1感染,而相同年龄的转基因小鼠和经玻璃体内注射IFN-γ处理的非转基因小鼠存活。眼部IFN-γ的产生增加了转基因小鼠的炎症程度,但直到接种后第3天对HSV-1的生长没有显著影响,也不影响该病毒的神经侵袭。因此,IFN-γ的作用不是由病毒复制的早期阻断引起的。IFN-γ作用的可能机制包括免疫反应的激活、病毒特性的改变以及对神经元的直接保护。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5228/236956/8b7ec4f2709c/jvirol00018-0235-a.jpg

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