VP1 codon deoptimization and high-fidelity substitutions in 3D polymerase as potential vaccine strategies for eliciting immune responses against enterovirus A71.
Wen-Sheng HsiehChiao-Hsuan ChaoChun-Yu ShenDayna ChengSheng-Wen HuangYa-Fang WangChien-Chin ChenShun-Hua ChenLi-Jin HsuJen-Ren WangPublished in: Journal of virology (2024)
EV-A71 can cause severe neurological diseases and cause death in young children. Here, we report the development of synthetic rgEV-A71s with the combination of codon deoptimization and high-fidelity (HF) substitutions that generate genetically stable reverse genetics (rg) viruses as potential attenuated vaccine candidates. Our work provides insight into the development of low-virulence candidate vaccines through a series of viral genetic editing for maintaining antigenicity and genome stability and suggests a strategy for the development of an innovative next-generation vaccine against EV-A71.