Your search keyword '"Liu, Rui-Lun"' showing total 3 results

1. Measles Virus-Based Vaccine Expressing Membrane-Anchored Spike of SARS-CoV-2 Inducing Efficacious Systemic and Mucosal Humoral Immunity in Hamsters.

Author

Yang, Zhi-Hui, Song, Yan-Li, Pei, Jie, Li, Song-Zhuang, Liu, Rui-Lun, Xiong, Yu, Wu, Jie, Liu, Yuan-Lang, Fan, Hui-Fen, Wu, Jia-Hui, Wang, Ze-Jun, Guo, Jing, Meng, Sheng-Li, Chen, Xiao-Qi, Lu, Jia, and Shen, Shuo

Subjects

SARS-CoV-2 Omicron variant, HUMORAL immunity, MEASLES vaccines, SARS-CoV-2, GOLDEN hamster, COVID-19

Abstract

As SARS-CoV-2 continues to evolve and COVID-19 cases rapidly increase among children and adults, there is an urgent need for a safe and effective vaccine that can elicit systemic and mucosal humoral immunity to limit the emergence of new variants. Using the Chinese Hu191 measles virus (MeV-hu191) vaccine strain as a backbone, we developed MeV chimeras stably expressing the prefusion forms of either membrane-anchored, full-length spike (rMeV-preFS), or its soluble secreted spike trimers with the help of the SP-D trimerization tag (rMeV-S+SPD) of SARS-CoV-2 Omicron BA.2. The two vaccine candidates were administrated in golden Syrian hamsters through the intranasal or subcutaneous routes to determine the optimal immunization route for challenge. The intranasal delivery of rMeV-S+SPD induced a more robust mucosal IgA antibody response than the subcutaneous route. The mucosal IgA antibody induced by rMeV-preFS through the intranasal routine was slightly higher than the subcutaneous route, but there was no significant difference. The rMeV-preFS vaccine stimulated higher mucosal IgA than the rMeV-S+SPD vaccine through intranasal or subcutaneous administration. In hamsters, intranasal administration of the rMeV-preFS vaccine elicited high levels of NAbs, protecting against the SARS-CoV-2 Omicron BA.2 variant challenge by reducing virus loads and diminishing pathological changes in vaccinated animals. Encouragingly, sera collected from the rMeV-preFS group consistently showed robust and significantly high neutralizing titers against the latest variant XBB.1.16. These data suggest that rMeV-preFS is a highly promising COVID-19 candidate vaccine that has great potential to be developed into bivalent vaccines (MeV/SARS-CoV-2). [ABSTRACT FROM AUTHOR]

Published

2024

2. Identification of Critical Amino Acids of Coxsackievirus A10 Associated with Cell Tropism and Viral RNA Release during Uncoating

Author

Pei, Jie, primary, Liu, Rui-Lun, additional, Yang, Zhi-Hui, additional, Du, Ya-Xin, additional, Qian, Sha-Sha, additional, Meng, Sheng-Li, additional, Guo, Jing, additional, Zhang, Bo, additional, and Shen, Shuo, additional

Published

2023

3. Humoral and cellular immunogenicity and efficacy of a coxsackievirus A10 vaccine in mice.

Author

An, Huan-Huan, Li, Meng, Liu, Rui-Lun, Wu, Jie, Meng, Sheng-Li, Guo, Jing, Wang, Ze-Jun, Qian, Sha-Sha, and Shen, Shuo

Published

2023