一种基于高度减毒痘苗病毒株LC16m8的严重发热伴血小板减少综合征疫苗。
A highly attenuated vaccinia virus strain LC16m8-based vaccine for severe fever with thrombocytopenia syndrome.
作者信息
Yoshikawa Tomoki, Taniguchi Satoshi, Kato Hirofumi, Iwata-Yoshikawa Naoko, Tani Hideki, Kurosu Takeshi, Fujii Hikaru, Omura Natsumi, Shibamura Miho, Watanabe Shumpei, Egawa Kazutaka, Inagaki Takuya, Sugimoto Satoko, Phanthanawiboon Supranee, Harada Shizuko, Yamada Souichi, Fukushi Shuetsu, Morikawa Shigeru, Nagata Noriyo, Shimojima Masayuki, Saijo Masayuki
机构信息
Department of Virology 1, National Institute of Infectious Diseases, Musashimurayama-shi, Tokyo, Japan.
Department of Pathology, National Institute of Infectious Diseases, Musashimurayama-shi, Tokyo, Japan.
出版信息
PLoS Pathog. 2021 Feb 3;17(2):e1008859. doi: 10.1371/journal.ppat.1008859. eCollection 2021 Feb.
Severe fever with thrombocytopenia syndrome (SFTS) caused by a species Dabie bandavirus (formerly SFTS virus [SFTSV]) is an emerging hemorrhagic infectious disease with a high case-fatality rate. One of the best strategies for preventing SFTS is to develop a vaccine, which is expected to induce both humoral and cellular immunity. We applied a highly attenuated but still immunogenic vaccinia virus strain LC16m8 (m8) as a recombinant vaccine for SFTS. Recombinant m8s expressing SFTSV nucleoprotein (m8-N), envelope glycoprotein precursor (m8-GPC), and both N and GPC (m8-N+GPC) in the infected cells were generated. Both m8-GPC- and m8-N+GPC-infected cells were confirmed to produce SFTSV-like-particles (VLP) in vitro, and the N was incorporated in the VLP produced by the infection of cells with m8-N+GPC. Specific antibodies to SFTSV were induced in mice inoculated with each of the recombinant m8s, and the mice were fully protected from lethal challenge with SFTSV at both 103 TCID50 and 105 TCID50. In mice that had been immunized with vaccinia virus strain Lister in advance of m8-based SFTSV vaccine inoculation, protective immunity against the SFTSV challenge was also conferred. The pathological analysis revealed that mice immunized with m8-GPC or m8-N+GPC did not show any histopathological changes without any viral antigen-positive cells, whereas the control mice showed focal necrosis with inflammatory infiltration with SFTSV antigen-positive cells in tissues after SFTSV challenge. The passive serum transfer experiments revealed that sera collected from mice inoculated with m8-GPC or m8-N+GPC but not with m8-N conferred protective immunity against lethal SFTSV challenge in naïve mice. On the other hand, the depletion of CD8-positive cells in vivo did not abrogate the protective immunity conferred by m8-based SFTSV vaccines. Based on these results, the recombinant m8-GPC and m8-N+GPC were considered promising vaccine candidates for SFTS.
由大别带病毒属(以前的发热伴血小板减少综合征病毒[SFTSV])引起的发热伴血小板减少综合征(SFTS)是一种新出现的、病死率很高的出血性传染病。预防SFTS的最佳策略之一是研发一种疫苗,预期该疫苗能诱导体液免疫和细胞免疫。我们应用一种高度减毒但仍具有免疫原性的痘苗病毒株LC16m8(m8)作为SFTS的重组疫苗。在感染细胞中产生了表达SFTSV核蛋白(m8-N)、包膜糖蛋白前体(m8-GPC)以及N和GPC两者(m8-N+GPC)的重组m8。已证实,感染m8-GPC和m8-N+GPC的细胞在体外均产生SFTSV样颗粒(VLP),并且N被整合到感染m8-N+GPC的细胞所产生的VLP中。接种每种重组m8的小鼠体内均诱导出了针对SFTSV的特异性抗体,并且这些小鼠对103 TCID50和105 TCID50的SFTSV致死性攻击均具有完全的保护作用。在用痘苗病毒株利斯特预先免疫的小鼠中接种基于m8的SFTSV疫苗后,也赋予了其针对SFTSV攻击的保护性免疫。病理分析显示,接种m8-GPC或m8-N+GPC的小鼠未表现出任何组织病理学变化,也未出现任何病毒抗原阳性细胞,而对照小鼠在受到SFTSV攻击后,其组织中出现了局灶性坏死并伴有炎症浸润以及SFTSV抗原阳性细胞。被动血清转移实验显示,从接种m8-GPC或m8-N+GPC而非m8-N的小鼠中收集的血清赋予了未免疫小鼠针对致死性SFTSV攻击的保护性免疫。另一方面,体内CD8阳性细胞的耗竭并未消除基于m8的SFTSV疫苗所赋予的保护性免疫。基于这些结果,重组m8-GPC和m8-N+GPC被认为是SFTS很有前景的候选疫苗。
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