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基于外泌体的VP1蛋白递送增强了小鼠对柯萨奇病毒B3诱导的病毒性心肌炎的抵抗力。

Exosome-based delivery of VP1 protein conferred enhanced resistance of mice to CVB3-induced viral myocarditis.

作者信息

Zhang Changwei, Zhang Yu, Li Yuanyu, Lu Juan, Xiong Sidong, Yue Yan

机构信息

Jiangsu Key Laboratory of Infection and Immunity, Institutes of Biology and Medical Sciences, Soochow University, Suzhou, China.

Jiangsu Key Laboratory of Infection and Immunity, Institutes of Biology and Medical Sciences, Soochow University, Suzhou, China.

出版信息

Virology. 2023 Feb;579:46-53. doi: 10.1016/j.virol.2022.12.015. Epub 2023 Jan 2.

Abstract

Coxsackievirus B3 (CVB3) is an important cause of viral myocarditis with no vaccine available in clinic. Herein we constructed an exosome-based anti-CVB3 vaccine (Exo-VP1), and compared its immunogenicity and immunoprotection with our previously reported recombinant VP1 protein (rVP1) vaccine. We found that compared with the 25 μg rVP1 vaccine, Exo-VP1 vaccine containing only 2 μg VP1 protein induced much stronger CVB3-specific T cell proliferation and CTL responses (with an increase of more than 70% and 40% respectively), and elicited greater splenic Th1/CTL associated cytokines (IFN-γ, TNF-α and IL-12). Furthermore, higher IgG levels with increased neutralizing titers and avidity were also evidenced in Exo-VP1 group. Consistently, Exo-VP1 group exhibited enhanced resistance to viral myocarditis than rVP1 vaccine, reflected by reduced cardiac viral loads, improved myocardial inflammation and an increased survival rate. Collectively, we reported that Exo-VP1 might present a more potent CVB3 vaccine candidate than rVP1 vaccine.

摘要

柯萨奇病毒B3(CVB3)是病毒性心肌炎的重要病因,临床上尚无可用疫苗。在此,我们构建了一种基于外泌体的抗CVB3疫苗(Exo-VP1),并将其免疫原性和免疫保护作用与我们之前报道的重组VP1蛋白(rVP1)疫苗进行了比较。我们发现,与25μg rVP1疫苗相比,仅含2μg VP1蛋白的Exo-VP1疫苗诱导出更强的CVB3特异性T细胞增殖和CTL反应(分别增加超过70%和40%),并引发更多的脾脏Th1/CTL相关细胞因子(IFN-γ、TNF-α和IL-12)。此外,Exo-VP1组还表现出更高的IgG水平,中和滴度和亲和力增加。同样,Exo-VP1组对病毒性心肌炎的抵抗力比rVP1疫苗增强,表现为心脏病毒载量降低、心肌炎症改善和存活率提高。总体而言,我们报道Exo-VP1可能是一种比rVP1疫苗更有效的CVB3疫苗候选物。

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