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携带靶向病毒糖蛋白的仙台病毒颗粒用于诱导抗体。

Sendai virus particles carrying target virus glycoproteins for antibody induction.

机构信息

AIDS Research Center, National Institute of Infectious Diseases, Tokyo 162-8640, Japan.

ID Pharma Co., Ltd., Ibaraki 300-2611, Japan.

出版信息

Vaccine. 2022 Apr 6;40(16):2420-2431. doi: 10.1016/j.vaccine.2022.03.008. Epub 2022 Mar 16.

DOI:10.1016/j.vaccine.2022.03.008
PMID:35305826
Abstract

Induction of antibodies targeting viral glycoproteins is a key for the development of a vaccine against enveloped virus infection. Glycoproteins on the virion exhibiting native multimer structure may be a good immunogen to present antibody epitopes, but it is often difficult to prepare immunogenic inactivated virions. Preparation of soluble glycoprotein multimers has been attempted, while virus-like particles carrying target glycoproteins can be a more immunogenic antigen. In the present study, a target glycoprotein-embedded Sendai virus (SeV) particle was developed for induction of anti-virus antibodies. We constructed a chimeric antigen, HIV-1 EnvF, consisting of HIV-1 Env ectodomain and SeV F transmembrane-cytoplasmic domain, which was shown to be efficiently incorporated into the SeV virion. EnvF was recognized by anti-HIV-1 broadly-neutralizing monoclonal antibodies (bnAbs) including 35O22 that targets an Env trimer-dependent epitope. Analysis revealed that HIV-1 EnvF can mediate viral entry into the cells, which is inhibited by anti-HIV-1 bnAbs and HIV-1 entry inhibitors, suggesting that the EnvF exhibits an HIV-1 Env native-like functional structure to present bnAb epitopes. Immunization of mice with replication-defective SeVs expressing HIV EnvF and non-infectious SeV particles (NVP) carrying HIV EnvF efficiently induced anti-HIV Env antibodies. HTLV-1 EnvF also showed the potential to efficiently induce anti-HTLV-1 Env antibodies. These results indicate that SeV particles carrying EnvF can be a promising vaccine platform for induction of antibodies targeting enveloped virus glycoproteins.

摘要

诱导针对病毒糖蛋白的抗体是开发针对包膜病毒感染疫苗的关键。展示天然多聚体结构的病毒粒子上的糖蛋白可能是呈现抗体表位的良好免疫原,但通常难以制备具有免疫原性的灭活病毒粒子。已经尝试制备可溶性糖蛋白多聚体,而携带靶糖蛋白的病毒样颗粒可以作为更具免疫原性的抗原。在本研究中,我们开发了一种含有靶向糖蛋白的仙台病毒(SeV)颗粒,用于诱导抗病毒抗体。我们构建了一种嵌合抗原 HIV-1 EnvF,由 HIV-1 Env 外域和 SeV F 跨膜-细胞质域组成,该抗原可有效地掺入 SeV 病毒粒子中。EnvF 被抗 HIV-1 的广泛中和单克隆抗体(bnAbs)识别,包括针对 Env 三聚体依赖性表位的 35O22。分析表明,HIV-1 EnvF 可以介导病毒进入细胞,这被抗 HIV-1 的 bnAbs 和 HIV-1 进入抑制剂抑制,表明 EnvF 表现出 HIV-1 Env 天然样功能结构以呈现 bnAb 表位。用表达 HIV EnvF 的复制缺陷型 SeV 和携带 HIV EnvF 的非感染性 SeV 颗粒(NVP)免疫小鼠,有效地诱导了抗 HIV Env 抗体。HTLV-1 EnvF 也显示出有效诱导抗 HTLV-1 Env 抗体的潜力。这些结果表明,携带 EnvF 的 SeV 颗粒可以成为诱导针对包膜病毒糖蛋白抗体的有前途的疫苗平台。

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