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用免疫球蛋白或阿昔洛韦治疗单纯疱疹病毒1型感染:比较它们对病毒传播、潜伏和再激活的影响。

Treatment of HSV-1 infection with immunoglobulin or acyclovir: comparison of their effects on viral spread, latency, and reactivation.

作者信息

LeBlanc R A, Pesnicak L, Godleski M, Straus S E

机构信息

Laboratory of Clinical Investigation, National Institutes of Health, Bethesda, Maryland 20892-1888, USA.

出版信息

Virology. 1999 Sep 15;262(1):230-6. doi: 10.1006/viro.1999.9891.

Abstract

We compared immunoglobulin (IgG) and acyclovir (ACV) therapies on the establishment, maintenance, and reactivation from latency of HSV-1(McKrae) in a mouse ocular infection model. Mice were given one intraperitoneal (IP) dose of human IgG 24 h after infection (Day 1 p. i.) or ACV in the drinking water from Days 1 to 7 p.i. Both treatments allowed similar percentages of mice to survive the infection and decreased ocular virus shedding as compared with untreated controls. At most time points, there were no differences between IgG- and ACV-treated animals with respect to tissue virus titers or in the rates of virus reactivation during explant cocultivation. However, after ultraviolet exposure, HSV reactivated in 30% of ACV-treated mice compared with 90% of IgG-treated mice (P = 0.02). Also by quantitative PCR, we found more latent HSV-1 DNA copies in IgG-treated mice compared with those given ACV (P = 0.02). IgG treatment protects mice from HSV-1 infection essentially as well as ACV does. Nonetheless, it permits higher levels of latent infection and subsequent in vivo reactivation. These studies have implications for the mechanism by which IgG functions to attenuate HSV infections and for its potential value as a therapeutic agent in humans.

摘要

我们在小鼠眼部感染模型中比较了免疫球蛋白(IgG)和阿昔洛韦(ACV)疗法对单纯疱疹病毒1型(McKrae株)潜伏状态的建立、维持及再激活的影响。感染后24小时(感染后第1天)给小鼠腹腔注射一剂人IgG,或者在感染后第1天至第7天让小鼠饮用含阿昔洛韦的水。与未治疗的对照组相比,两种治疗方法都使相似比例的小鼠在感染中存活下来,并减少了眼部病毒脱落。在大多数时间点,接受IgG和ACV治疗的动物在组织病毒滴度或外植体共培养期间的病毒再激活率方面没有差异。然而,紫外线照射后,30%接受ACV治疗的小鼠出现了HSV再激活,而接受IgG治疗的小鼠这一比例为90%(P = 0.02)。通过定量PCR我们还发现,与接受ACV治疗的小鼠相比,接受IgG治疗的小鼠体内潜伏的HSV-1 DNA拷贝更多(P = 0.02)。IgG治疗对小鼠HSV-1感染的保护作用基本与ACV相当。尽管如此,它会导致更高水平的潜伏感染和随后的体内再激活。这些研究对IgG减轻HSV感染的作用机制及其作为人类治疗药物的潜在价值具有启示意义。

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