Rational design of self-amplifying virus-like vesicles with Ebola virus glycoprotein as vaccines

埃博拉病毒 病毒学 糖蛋白 病毒 合理设计 生物 分子生物学 遗传学
作者
Hongqing Zhang,Yanan Zhang,Cheng‐Lin Deng,Qin-Xuan Zhu,Zhe-Rui Zhang,Xiaodan Li,Zhiming Yuan,Bo Zhang
出处
期刊:Molecular Therapy [Elsevier BV]
卷期号:32 (10): 3695-3711
标识
DOI:10.1016/j.ymthe.2024.08.026
摘要

As emerging and re-emerging pathogens, filoviruses, especially Ebola virus (EBOV), pose a great threat to public health and require sustained attention and ongoing surveillance. More vaccines and antiviral drugs are imperative to be developed and stockpiled to respond to unpredictable outbreaks. Virus-like vesicles, generated by alphavirus replicons expressing homogeneous or heterogeneous glycoproteins (GPs), have demonstrated the capacity of self-propagation and shown great potential in vaccine development. Here, we describe a novel class of EBOV-like vesicles (eVLVs) incorporating both EBOV GP and VP40. The eVLVs exhibited similar antigenicity as EBOV. In murine models, eVLVs were highly attenuated and elicited robust GP-specific antibodies with neutralizing activities. Importantly, a single dose of eVLVs conferred complete protection in a surrogate EBOV lethal mouse model. Furthermore, our VLVs strategy was also successfully applied to Marburg virus (MARV), the representative member of the genus Marburgvirus. Taken together, our findings indicate the feasibility of an alphavirus-derived VLVs strategy in combating infection of filoviruses represented by EBOV and MARV, which provides further evidence of the potential of this platform for universal live-attenuated vaccine development.
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