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用一种活的、温度敏感的重组流感病毒对小鼠进行气溶胶疫苗接种。

Aerosol vaccination of mice with a live, temperature- sensitive recombinant influenza virus.

作者信息

Jemski J V, Walker J S

出版信息

Infect Immun. 1976 Mar;13(3):818-24. doi: 10.1128/iai.13.3.818-824.1976.

Abstract

Mice were vaccinated intranasally (i.n.) or with small-particle aerosols (SPA; 2 mum) or large-particle aerosols (LPA; 8 mum) of an attenuated, temperature-sensitive, recombinant A influenza (H3N2) virus, ts-1 (E). Serum virus-neutralizing and hemagglutination inhibition antibodies were detected for all vaccinated mice by 28 days. Bronchoalveolar wash fluids had increased levels of immunoglobulin (IgG, IgA) only in the i.n. -vaccinated mice. Hemagglutination and virus-neutralizing antibodies were detected in the SPA- and i.n. -vaccinated groups but not in the LPA vaccinates. Upon challenge with SPA of a mouse virulent H3N2 influenza vitus, total protection was obtained for the SPA- and I.N. -vaccinated mice, whereas only 89% of the LPA group survived. Replication of the challenge virus was signifcantly repressed in both the lower and upper respiratory tracts of the three groups of vaccinated mice compared to the nonvaccinated controls. The protection afforded the SPA- and i.n. -vaccinated mice was the same as measured for mice after recovery from earlier subelthal active infection with virulent virus.

摘要

用减毒、温度敏感的重组甲型流感(H3N2)病毒ts-1(E)对小鼠进行鼻内(i.n.)接种,或用小颗粒气溶胶(SPA;2微米)或大颗粒气溶胶(LPA;8微米)接种。到28天时,检测到所有接种小鼠的血清病毒中和抗体和血凝抑制抗体。仅在鼻内接种的小鼠支气管肺泡灌洗液中免疫球蛋白(IgG、IgA)水平升高。在SPA接种组和鼻内接种组中检测到血凝和病毒中和抗体,但在LPA接种组中未检测到。在用小鼠强毒H3N2流感病毒的SPA攻击后,SPA接种组和鼻内接种组的小鼠获得了完全保护,而LPA组只有89%存活。与未接种对照相比,在三组接种小鼠的上、下呼吸道中,攻击病毒的复制均受到显著抑制。对SPA接种组和鼻内接种组小鼠的保护作用与从早期亚致死性强毒病毒主动感染中恢复后的小鼠所测得的保护作用相同。

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