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Effects of immunosuppression with cyclophosphamide on acute murine cytomegalovirus infection and virus-augmented natural killer cell activity.

机译:免疫抑制与环磷酰胺对急性小鼠胞嘧啶胞嘧啶感染和病毒增强自然杀伤细胞活性的影响。

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The effects of cyclophosphamide (CY) treatment on acute murine cytomegalovirus (MCMV) infection were studied to explore the potential usefulness of MCMV as a means of detecting immune dysfunction and to identify host defense mechanisms important for protection against MCMV. Conditions found optimal for enhancing MCMV infection with CY included infecting adult mice with 2 X 10(5) PFU or more of virus and administering 80 mg or more of CY per kg 1 to 3 days later. In addition to enhanced mortality, virus titers in lung, liver, and spleen were elevated in CY-treated mice, and wet weights of liver, spleen, and thymus were depressed when compared with those of infected but untreated mice. Treatment with CY before MCMV challenge was not as efficient a means of enhancing mortality as treatment after virus challenge. The effect that the time of CY administration relative to infection had on mortality correlated with the effect of such timing on natural killer cell activity. Animals treated before infection exhibited depressed natural killer cell activity initially. However, they rapidly recovered this response, and by 5 days postinfection they had the same level of virus-augmented activity seen in untreated mice. In contrast, animals treated after infection did not recover natural killer cell activity and were more likely to die. A similar correlation was not obtained when the effects of CY on lymphocyte responses to B and T cell mitogens were examined, nor were there striking differences in pathology between the treatment groups. The data suggest an important role for natural killer cells in host defense against MCMV. Also, increased susceptibility to MCMV may provide a useful indicator of deficits in the natural killer cell response.
机译:研究了环磷酰胺(CY)处理对急性小鼠胞嘧啶病毒(MCMV)感染的影响,探讨MCMV作为检测免疫功能障碍的手段的潜在有用性,并鉴定对MCMV保护重要的主体防御机制。用于增强具有2×10(5)个PFU或更多病毒的成人小鼠的Cy的MCMV感染的条件是最佳的最佳状态最佳,并在1至3天后施用80mg或更多的Cy。除了增强的死亡率外,肺,肝脏和脾脏中的病毒滴度在与感染但未经处理的小鼠的小鼠相比时抑制了肝脏,脾和胸腺的湿重。在MCMV挑战之前用Cy治疗并不是在病毒攻击后加强死亡率的方法,以提高死亡率。 Cy施用时间相对于感染的效果对死亡率的影响与自然杀手细胞活性的这种时序的影响相关。感染前治疗的动物最初表现出抑郁的自然杀伤细胞活性。然而,它们迅速恢复了这种反应,并且在未经治疗的小鼠中患有相同的病毒增强活性,在5天内恢复过来。相比之下,感染后治疗的动物没有恢复自然杀手细胞活性,并且更可能死亡。当检查CY对B和T细胞丝率的淋巴细胞反应的效果时,未获得类似的相关性,治疗组之间的病理学差异也没有显着差异。该数据表明对MCMV宿主防御中的自然杀伤细胞的重要作用。此外,对MCMV的易感性增加可以提供自然杀伤细胞反应中的有用指标。

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