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一种优化的 FI-RSV 疫苗可有效保护棉鼠和 BALB/c 小鼠,而不会引起增强的呼吸道疾病。

An Optimized FI-RSV Vaccine Effectively Protects Cotton Rats and BALB/c Mice without Causing Enhanced Respiratory Disease.

机构信息

State Key Laboratory of Molecular Vaccinology and Molecular Diagnostics, National Institute of Diagnostics and Vaccine Development in Infectious Diseases, School of Public Health, Xiamen University, Xiamen 361002, China.

出版信息

Viruses. 2022 Sep 20;14(10):2085. doi: 10.3390/v14102085.

Abstract

BACKGROUND

Despite considerable efforts toward vaccine development in past decades, no effective vaccines against respiratory syncytial virus (RSV) are available. Recently, we showed that an optimized formalin concentration can preserve prefusion protein (pre-F) on RSV-infected cells and protect mice against RSV infection without causing enhanced respiratory disease (ERD). Here, we sought to further stabilize pre-F on RSV virions by optimizing the production of FI-RSV.

METHODS

Freshly produced RSV virions were treated with formalin under different concentrations to obtained an opti-FI-RSV vaccine with high pre-F level. Immunogenicity and safety of opti-FI-RSV were evaluated in Balb/c mice and cotton rats.

RESULTS

Using 0.0156-0.1778% formalin, we successfully preserved pre-F on virions. This opti-FI-RSV exhibited improved immunogenicity and efficacy without causing ERD. Surprisingly, opti-FI-RSV, with a pre-F-dominant immunogen, still caused ERD after immunization with a suboptimal dose or when the neutralizing antibody titers declined. ERD was avoided by coadministering opti-FI-RSV with CpG + MPLA adjuvant, which subsequently induced a Th1-biasing immune response and, more importantly, significantly improved antibody avidity.

CONCLUSIONS

Our study provides a new method to obtain a novel FI-RSV vaccine with a high pre-F level and may provide a reference for developing other inactivated vaccines. Our findings also emphasize that appropriate adjuvants are critical for nonreplicating vaccines.

摘要

背景

尽管过去几十年在疫苗开发方面做出了相当大的努力,但仍没有针对呼吸道合胞病毒(RSV)的有效疫苗。最近,我们发现优化的福尔马林浓度可以保留 RSV 感染细胞上的融合前蛋白(pre-F),并在不引起增强性呼吸道疾病(ERD)的情况下保护小鼠免受 RSV 感染。在此,我们通过优化 FI-RSV 的生产来进一步稳定 RSV 病毒粒子上的 pre-F。

方法

用不同浓度的福尔马林处理新产生的 RSV 病毒粒子,以获得高水平 pre-F 的 opti-FI-RSV 疫苗。在 Balb/c 小鼠和棉鼠中评估 opti-FI-RSV 的免疫原性和安全性。

结果

使用 0.0156-0.1778%的福尔马林,我们成功地将 pre-F 保留在病毒粒子上。这种 opti-FI-RSV 表现出改善的免疫原性和疗效,而不会引起 ERD。令人惊讶的是,opt-FI-RSV 虽然具有 pre-F 优势免疫原性,但在免疫接种亚最佳剂量或中和抗体滴度下降后仍会引起 ERD。通过与 CpG+MPLA 佐剂共同给药来避免 ERD,这随后诱导了 Th1 偏向性免疫反应,更重要的是,显著提高了抗体亲和力。

结论

我们的研究提供了一种获得高 pre-F 水平的新型 FI-RSV 疫苗的新方法,可为开发其他灭活疫苗提供参考。我们的研究结果还强调了适当的佐剂对于非复制疫苗的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2332/9612074/a3039fa3a245/viruses-14-02085-g001.jpg

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