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用灭活呼吸道合胞病毒经鼻/口联合免疫后小鼠的快速恢复。

Rapid recovery in mice after combined nasal/oral immunization with killed respiratory syncytial virus.

作者信息

Reuman P D, Keely S P, Schiff G M

机构信息

James N. Gamble Institute of Medical Research, Cincinnati, Ohio 45219.

出版信息

J Med Virol. 1990 Sep;32(1):67-72. doi: 10.1002/jmv.1890320112.

Abstract

Based on the concept of a common mucosal immune system, the murine gastrointestinal tract was inoculated (oral) with three doses (5, 20, and 40 micrograms) of UV-inactivated respiratory syncytial virus (RSV) in order to elicit a virus-specific immune response in the respiratory tract. Only the 40 micrograms dose induced significant (P less than 0.01) anti-RSV-IgG rises in serum and lung wash compared to controls. To improve the immune response, mice were immunized intranasally under light anesthesia with the same 40 micrograms dosage regimen of killed RSV so that each dose passed through the nose and was swallowed. This combined nasal/oral immunization stimulated anti-RSV-IgG in serum, lung wash and nasal wash (P less than 0.001) and anti-RSV-IgA in lung and nasal wash (P less than 0.001) that were comparable to levels after infection with live RSV. Three days after challenge with live RSV, mice given combined nasal/oral immunization showed suppressed nasal virus shedding (P = 0.025). Nasal virus shedding correlated inversely with concentrations of anti-RSV-Ig in nasal secretions but did not correlate with concentrations in serum.

摘要

基于共同黏膜免疫系统的概念,给小鼠胃肠道进行口服接种三剂(5微克、20微克和40微克)紫外线灭活的呼吸道合胞病毒(RSV),以便在呼吸道引发病毒特异性免疫反应。与对照组相比,只有40微克剂量组血清和肺灌洗液中的抗RSV-IgG出现显著升高(P<0.01)。为了增强免疫反应,在轻度麻醉下给小鼠进行鼻内免疫,采用相同的40微克剂量方案的灭活RSV,使每剂药物经鼻进入并被吞咽。这种鼻内/口服联合免疫刺激血清、肺灌洗液和鼻洗液中的抗RSV-IgG(P<0.001)以及肺和鼻洗液中的抗RSV-IgA(P<0.001),其水平与感染活RSV后的水平相当。用活RSV攻击三天后,接受鼻内/口服联合免疫的小鼠鼻内病毒排出受到抑制(P=0.025)。鼻内病毒排出与鼻分泌物中抗RSV-Ig的浓度呈负相关,但与血清中的浓度无关。

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