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一种用于克里米亚-刚果出血热的DNA疫苗在两种致死性小鼠模型中可预防疾病和死亡。

A DNA vaccine for Crimean-Congo hemorrhagic fever protects against disease and death in two lethal mouse models.

作者信息

Garrison Aura R, Shoemaker Charles J, Golden Joseph W, Fitzpatrick Collin J, Suschak John J, Richards Michelle J, Badger Catherine V, Six Carolyn M, Martin Jacqueline D, Hannaman Drew, Zivcec Marko, Bergeron Eric, Koehler Jeffrey W, Schmaljohn Connie S

机构信息

Virology Division, United States Army Medical Research Institute of Infectious Diseases, Fort Detrick, Maryland, United States of America.

Ichor Medical Systems, Inc., San Diego, California, United States of America.

出版信息

PLoS Negl Trop Dis. 2017 Sep 18;11(9):e0005908. doi: 10.1371/journal.pntd.0005908. eCollection 2017 Sep.

Abstract

Crimean-Congo hemorrhagic fever virus (CCHFV) is a tick-borne virus capable of causing a severe hemorrhagic fever disease in humans. There are currently no licensed vaccines to prevent CCHFV-associated disease. We developed a DNA vaccine expressing the M-segment glycoprotein precursor gene of CCHFV and assessed its immunogenicity and protective efficacy in two lethal mouse models of disease: type I interferon receptor knockout (IFNAR-/-) mice; and a novel transiently immune suppressed (IS) mouse model. Vaccination of mice by muscle electroporation of the M-segment DNA vaccine elicited strong antigen-specific humoral immune responses with neutralizing titers after three vaccinations in both IFNAR-/- and IS mouse models. To compare the protective efficacy of the vaccine in the two models, groups of vaccinated mice (7-10 per group) were intraperitoneally (IP) challenged with a lethal dose of CCHFV strain IbAr 10200. Weight loss was markedly reduced in CCHFV DNA-vaccinated mice as compared to controls. Furthermore, whereas all vector-control vaccinated mice succumbed to disease by day 5, the DNA vaccine protected >60% of the animals from lethal disease. Mice from both models developed comparable levels of antibodies, but the IS mice had a more balanced Th1/Th2 response to vaccination. There were no statistical differences in the protective efficacies of the vaccine in the two models. Our results provide the first comparison of these two mouse models for assessing a vaccine against CCHFV and offer supportive data indicating that a DNA vaccine expressing the glycoprotein genes of CCHFV elicits protective immunity against CCHFV.

摘要

克里米亚-刚果出血热病毒(CCHFV)是一种蜱传病毒,可导致人类患上严重的出血热疾病。目前尚无预防CCHFV相关疾病的许可疫苗。我们研发了一种表达CCHFV M片段糖蛋白前体基因的DNA疫苗,并在两种致死性小鼠疾病模型中评估了其免疫原性和保护效力:I型干扰素受体敲除(IFNAR-/-)小鼠;以及一种新型的短暂免疫抑制(IS)小鼠模型。在IFNAR-/-和IS小鼠模型中,通过肌肉电穿孔接种M片段DNA疫苗的小鼠在三次接种后均引发了强烈的抗原特异性体液免疫反应,并产生了中和抗体滴度。为了比较该疫苗在两种模型中的保护效力,将接种疫苗的小鼠组(每组7-10只)腹腔内(IP)注射致死剂量的CCHFV IbAr 10200毒株进行攻毒。与对照组相比,接种CCHFV DNA疫苗的小鼠体重减轻明显减少。此外,虽然所有接种载体对照疫苗的小鼠在第5天均死于疾病,但DNA疫苗保护了>60%的动物免于致死性疾病。两种模型中的小鼠产生的抗体水平相当,但IS小鼠对疫苗接种的Th1/Th2反应更为平衡。该疫苗在两种模型中的保护效力没有统计学差异。我们的结果首次比较了这两种用于评估抗CCHFV疫苗的小鼠模型,并提供了支持性数据,表明表达CCHFV糖蛋白基因的DNA疫苗可引发针对CCHFV的保护性免疫。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c773/5619839/74159c7b1c27/pntd.0005908.g001.jpg

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