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一种腺病毒载体裂谷热疫苗可使A129小鼠完全抵御致死性裂谷热病毒攻击。

An adenovirus-vectored RVF vaccine confers complete protection against lethal RVFV challenge in A129 mice.

作者信息

Hao Meng, Bian Ting, Fu Guangcheng, Chen Yi, Fang Ting, Zhao Chuanyi, Liu Shuling, Yu Changming, Li Jianmin, Chen Wei

机构信息

Vaccine and Antibody Engineer Laboratory, Beijing Institute of Biotechnology, Beijing, China.

Frontier Biotechnology Laboratory, Zhejiang University-Hangzhou Global Scientific and Technological Innovation Center, Hangzhou, China.

出版信息

Front Microbiol. 2023 Feb 28;14:1114226. doi: 10.3389/fmicb.2023.1114226. eCollection 2023.

Abstract

Rift valley fever virus (RVFV) is a mosquito-transmitted bunyavirus that causes severe disease in animals and humans. Nevertheless, there are no vaccines applied to prevent RVFV infection for human at present. Therefore, it is necessary to develop a safe and effective RVFV vaccine. We generated Ad5-GnGcopt, a replication-deficient recombinant Ad5 vector (human adenovirus serotype 5) expressing codon-optimized RVFV glycoproteins Gn and Gc, and evaluated its immunogenicity and protective efficacy in mice. Intramuscular immunization of Ad5-GnGcopt in mice induces strong and durable antibody production and robust cellular immune responses. Additionally, a single vaccination with Ad5-GnGcopt vaccination can completely protect interferon-α/β receptor-deficient A129 mice from lethal RVFV infection. Our work indicates that Ad5-GnGcopt might represent a potential vaccine candidate against RVFV. However, further research is needed, first to confirm its efficacy in a natural animal host, and ultimately escalate as a potential vaccine candidate for humans.

摘要

裂谷热病毒(RVFV)是一种通过蚊子传播的布尼亚病毒,可在动物和人类中引发严重疾病。然而,目前尚无用于预防人类RVFV感染的疫苗。因此,有必要开发一种安全有效的RVFV疫苗。我们构建了Ad5-GnGcopt,这是一种复制缺陷型重组Ad5载体(人腺病毒血清型5),表达密码子优化的RVFV糖蛋白Gn和Gc,并在小鼠中评估了其免疫原性和保护效果。在小鼠中肌肉注射Ad5-GnGcopt可诱导强烈且持久的抗体产生以及强大的细胞免疫反应。此外,单次接种Ad5-GnGcopt疫苗可完全保护缺乏干扰素-α/β受体的A129小鼠免受致命的RVFV感染。我们的研究表明,Ad5-GnGcopt可能是一种潜在的抗RVFV疫苗候选物。然而,还需要进一步研究,首先要在天然动物宿主中确认其有效性,并最终作为人类潜在的疫苗候选物进行升级。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/18da/10011166/3d9293ab4950/fmicb-14-1114226-g001.jpg

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