Crimean Congo hemorrhagic fever virus nucleoprotein and GP38 subunit vaccine combination prevents morbidity in mice.

IF 6.9 1区 医学 Q1 IMMUNOLOGY
Elif Karaaslan, Teresa E Sorvillo, Florine E M Scholte, Troy Justin O'Neal, Stephen R Welch, Katherine A Davies, JoAnn D Coleman-McCray, Jessica R Harmon, Jana M Ritter, Scott D Pegan, Joel M Montgomery, Jessica R Spengler, Christina F Spiropoulou, Éric Bergeron
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Abstract

Immunizing mice with Crimean-Congo hemorrhagic fever virus (CCHFV) nucleoprotein (NP), glycoprotein precursor (GPC), or with the GP38 domain of GPC, can be protective when the proteins are delivered with viral vectors or as a DNA or RNA vaccine. Subunit vaccines are a safe and cost-effective alternative to some vaccine platforms, but Gc and Gn glycoprotein subunit vaccines for CCHFV fail to protect despite eliciting high levels of neutralizing antibodies. Here, we investigated humoral and cellular immune responses and the protective efficacy of recombinant NP, GP38, and GP38 forms (GP85 and GP160) associated with the highly glycosylated mucin-like (MLD) domain, as well as the NP + GP38 combination. Vaccination with GP160, GP85, or GP38 did not confer protection, and vaccination with the MLD-associated GP38 forms blunted the humoral immune responses to GP38, worsened clinical chemistry, and increased viral RNA in the blood compared to the GP38 vaccination. In contrast, NP vaccination conferred 100% protection from lethal outcome and was associated with mild clinical disease, while the NP + GP38 combination conferred even more robust protection by reducing morbidity compared to mice receiving NP alone. Thus, recombinant CCHFV NP alone is a promising vaccine candidate conferring 100% survival against heterologous challenge. Moreover, incorporation of GP38 should be considered as it further enhances subunit vaccine efficacy by reducing morbidity in surviving animals.

Abstract Image

克里米亚刚果出血热病毒核蛋白和 GP38 亚基联合疫苗可预防小鼠发病。
用克里米亚-刚果出血热病毒(CCHFV)核蛋白(NP)、糖蛋白前体(GPC)或GPC的GP38结构域对小鼠进行免疫,当这些蛋白通过病毒载体或作为DNA或RNA疫苗递送时,可以起到保护作用。亚单位疫苗是某些疫苗平台的一种安全且具有成本效益的替代品,但针对CCHFV的Gc和Gn糖蛋白亚单位疫苗尽管能激发高水平的中和抗体,但却起不到保护作用。在这里,我们研究了重组 NP、GP38、与高度糖基化的粘蛋白样(MLD)结构域相关的 GP38 形式(GP85 和 GP160)以及 NP + GP38 组合的体液和细胞免疫反应及保护效力。与接种GP38疫苗相比,接种GP160、GP85或GP38疫苗不会产生保护作用,而接种与MLD相关的GP38形式则会减弱对GP38的体液免疫反应,使临床生化指标恶化,并增加血液中的病毒RNA。与此相反,NP疫苗接种可100%保护小鼠免于致死,且临床疾病轻微,而NP + GP38组合疫苗接种则可提供更强大的保护,与单独接种NP的小鼠相比,发病率更低。因此,单用重组 CCHFV NP 是一种很有前途的候选疫苗,可使小鼠在异源挑战中 100% 存活。此外,还应考虑加入 GP38,因为它能降低存活动物的发病率,从而进一步提高亚单位疫苗的功效。
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来源期刊
NPJ Vaccines
NPJ Vaccines Immunology and Microbiology-Immunology
CiteScore
11.90
自引率
4.30%
发文量
146
审稿时长
11 weeks
期刊介绍: Online-only and open access, npj Vaccines is dedicated to highlighting the most important scientific advances in vaccine research and development.
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