Cell Discovery (Feb 2022)
Design of a mutation-integrated trimeric RBD with broad protection against SARS-CoV-2
- Yu Liang,
- Jing Zhang,
- Run Yu Yuan,
- Mei Yu Wang,
- Peng He,
- Ji Guo Su,
- Zi Bo Han,
- Yu Qin Jin,
- Jun Wei Hou,
- Hao Zhang,
- Xue Feng Zhang,
- Shuai Shao,
- Ya Nan Hou,
- Zhao Ming Liu,
- Li Fang Du,
- Fu Jie Shen,
- Wei Min Zhou,
- Ke Xu,
- Ru Qin Gao,
- Fang Tang,
- Ze Hua Lei,
- Shuo Liu,
- Wei Zhen,
- Jin Juan Wu,
- Xiang Zheng,
- Ning Liu,
- Shi Chen,
- Zhi Jing Ma,
- Fan Zheng,
- Si Yu Ren,
- Zhong Yu Hu,
- Wei Jin Huang,
- Gui Zhen Wu,
- Chang Wen Ke,
- Qi Ming Li
Affiliations
- Yu Liang
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Jing Zhang
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Run Yu Yuan
- Guangdong Provincial Institute of Public Health, Guangdong Provincial Center for Disease Control and Prevention
- Mei Yu Wang
- National Institute for Food and Drug Control (NIFDC)
- Peng He
- National Institute for Food and Drug Control (NIFDC)
- Ji Guo Su
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Zi Bo Han
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Yu Qin Jin
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Jun Wei Hou
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Hao Zhang
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Xue Feng Zhang
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Shuai Shao
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Ya Nan Hou
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Zhao Ming Liu
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Li Fang Du
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Fu Jie Shen
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Wei Min Zhou
- National Institute for Viral Disease Control and Prevention, Chinese Center for Disease Control and Prevention (China CDC)
- Ke Xu
- National Institute for Viral Disease Control and Prevention, Chinese Center for Disease Control and Prevention (China CDC)
- Ru Qin Gao
- Qingdao Centers for Disease Control and Prevention
- Fang Tang
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Ze Hua Lei
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Shuo Liu
- National Institute for Food and Drug Control (NIFDC)
- Wei Zhen
- National Institute for Viral Disease Control and Prevention, Chinese Center for Disease Control and Prevention (China CDC)
- Jin Juan Wu
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Xiang Zheng
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Ning Liu
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Shi Chen
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Zhi Jing Ma
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Fan Zheng
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Si Yu Ren
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- Zhong Yu Hu
- National Institute for Food and Drug Control (NIFDC)
- Wei Jin Huang
- National Institute for Food and Drug Control (NIFDC)
- Gui Zhen Wu
- National Institute for Viral Disease Control and Prevention, Chinese Center for Disease Control and Prevention (China CDC)
- Chang Wen Ke
- Guangdong Provincial Institute of Public Health, Guangdong Provincial Center for Disease Control and Prevention
- Qi Ming Li
- The Sixth Laboratory, National Vaccine and Serum Institute (NVSI)
- DOI
- https://doi.org/10.1038/s41421-022-00383-5
- Journal volume & issue
-
Vol. 8,
no. 1
pp. 1 – 17
Abstract
Abstract The continuous emergence of SARS-CoV-2 variants highlights the need of developing vaccines with broad protection. Here, according to the immune-escape capability and evolutionary convergence, the representative SARS-CoV-2 strains carrying the hotspot mutations were selected. Then, guided by structural and computational analyses, we present a mutation-integrated trimeric form of spike receptor-binding domain (mutI-tri-RBD) as a broadly protective vaccine candidate, which combined heterologous RBDs from different representative strains into a hybrid immunogen and integrated immune-escape hotspots into a single antigen. When compared with a homo-tri-RBD vaccine candidate in the stage of phase II trial, of which all three RBDs are derived from the SARS-CoV-2 prototype strain, mutI-tri-RBD induced significantly higher neutralizing antibody titers against the Delta and Beta variants, and maintained a similar immune response against the prototype strain. Pseudo-virus neutralization assay demonstrated that mutI-tri-RBD also induced broadly strong neutralizing activities against all tested 23 SARS-CoV-2 variants. The in vivo protective capability of mutI-tri-RBD was further validated in hACE2-transgenic mice challenged by the live virus, and the results showed that mutI-tri-RBD provided potent protection not only against the SARS-CoV-2 prototype strain but also against the Delta and Beta variants.
