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在用编码日本脑炎病毒前膜和包膜基因的质粒进行疫苗接种后,记忆性中和抗体反应对于保护小鼠免受攻击至关重要。

The anamnestic neutralizing antibody response is critical for protection of mice from challenge following vaccination with a plasmid encoding the Japanese encephalitis virus premembrane and envelope genes.

作者信息

Konishi E, Yamaoka M, Kurane I, Takada K, Mason P W

机构信息

Department of Health Sciences, Kobe University School of Medicine, Kobe 654-0142, Japan.

出版信息

J Virol. 1999 Jul;73(7):5527-34. doi: 10.1128/JVI.73.7.5527-5534.1999.

Abstract

For Japanese encephalitis (JE), we previously reported that recombinant vaccine-induced protection from disease does not prevent challenge virus replication in mice. Moreover, DNA vaccines for JE can provide protection from high challenge doses in the absence of detectable prechallenge neutralizing antibodies. In the present study, we evaluated the role of postchallenge immune responses in determining the outcome of JE virus infection, using mice immunized with a plasmid, pcDNA3JEME, encoding the JE virus premembrane (prM) and envelope (E) coding regions. In the first experiment, 10 mice were vaccinated once (five animals) or twice (remainder) with 100 micrograms of pcDNA3JEME. All of these mice showed low (6 of 10) or undetectable (4 of 10) levels of neutralizing antibodies. Interestingly, eight of these animals showed a rapid rise in neutralizing antibody following challenge with 10,000 50% lethal doses of JE virus and survived for 21 days, whereas only one of the two remaining animals survived. No unimmunized animals exhibited a rise of neutralizing antibody or survived challenge. Levels of JE virus-specific immunoglobulin M class antibodies were elevated following challenge in half of the unimmunized mice and in the single pcDNA3JEME-immunized mouse that died. In the second experiment, JE virus-specific primary cytotoxic T-lymphocyte (CTL) activity was detected in BALB/c mice immunized once with 100 micrograms of pcDNA3JEME 4 days after challenge, indicating a strong postchallenge recall of CTLs. In the third experiment, evaluation of induction of CTLs and antibody activity by plasmids containing portions of the prM/E cassette demonstrated that induction of CTL responses alone were not sufficient to prevent death. Finally, we showed that antibody obtained from pcDNA3JEME-immunized mice 4 days following challenge could partially protect recipient mice from lethal challenge. Taken together, these results indicate that neutralizing antibody produced following challenge provides the critical protective component in pcDNA3JEME-vaccinated mice.

摘要

对于日本脑炎(JE),我们之前报道过重组疫苗诱导的疾病防护并不能阻止小鼠体内攻击病毒的复制。此外,针对JE的DNA疫苗在没有可检测到的攻击前中和抗体的情况下,能够抵御高剂量的攻击。在本研究中,我们使用用编码JE病毒前膜(prM)和包膜(E)编码区的质粒pcDNA3JEME免疫的小鼠,评估了攻击后免疫反应在决定JE病毒感染结果中的作用。在第一个实验中,10只小鼠用100微克的pcDNA3JEME进行一次(5只动物)或两次(其余动物)接种。所有这些小鼠的中和抗体水平都很低(10只中的6只)或检测不到(10只中的4只)。有趣的是,这些动物中有8只在用10,000个50%致死剂量的JE病毒攻击后,中和抗体迅速上升,并存活了21天,而其余两只动物中只有一只存活。未免疫的动物没有出现中和抗体的上升,也没有在攻击中存活。在一半未免疫的小鼠以及死亡的那只单次pcDNA3JEME免疫的小鼠中,攻击后JE病毒特异性免疫球蛋白M类抗体水平升高。在第二个实验中,在攻击后4天,在单次用100微克的pcDNA3JEME免疫的BALB/c小鼠中检测到了JE病毒特异性原发性细胞毒性T淋巴细胞(CTL)活性,表明攻击后CTL有强烈的回忆反应。在第三个实验中,对包含prM/E盒部分的质粒诱导CTL和抗体活性的评估表明,单独诱导CTL反应不足以防止死亡。最后,我们表明在攻击后4天从pcDNA3JEME免疫的小鼠中获得的抗体可以部分保护受体小鼠免受致死性攻击。综上所述,这些结果表明,攻击后产生的中和抗体是pcDNA3JEME接种小鼠中的关键保护成分。

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