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Rapid Development of SARS-CoV-2 Spike Protein Receptor-Binding Domain Self-Assembled Nanoparticle Vaccine Candidates

ACS Nano. 2021-02; 
Yin-Feng Kang, Cong Sun , Zhen Zhuang , Run-Yu Yuan , Qingbing Zheng , Jiang-Ping Li , Ping-Ping Zhou , Xin-Chun Chen , Zhe Liu , Xiao Zhang, Xiao-Hui Yu , Xiang-Wei Kong , Qian-Ying Zhu , Qian Zhong , Miao Xu , Nan-Shan Zhong , Yi-Xin Zeng , Guo-Kai Feng , Changwen Ke , Jin-Cun Zhao , Mu-Sheng Zeng
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Gene Synthesis The IgG heavy and light chain variable genes of CB6 mAb (GenBank: MT470196 and MT470197) were codon-optimized for human cells, synthesized by GenScript, and cloned into the antibody expression vector. Endotoxin was removed from all purified protein preparations using the ToxinEraser Endotoxin Removal Kit (GenScript) according to the manufacturer’s instructions. Get A Quote
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摘要

The coronavirus disease pandemic of 2019 (COVID-19) caused by the novel SARS-CoV-2 coronavirus resulted in economic losses and threatened human health worldwide. The pandemic highlights an urgent need for a stable, easily produced, and effective vaccine. SARS-CoV-2 uses the spike protein receptor-binding domain (RBD) to bind its cognate receptor, angiotensin-converting enzyme 2 (ACE2), and initiate membrane fusion. Thus, the RBD is an ideal target for vaccine development. In this study, we designed three different RBD-conjugated nanoparticle vaccine candidates, namely, RBD-Ferritin (24-mer), RBD-mi3 (60-mer), and RBD-I53-50 (120-mer), via covalent conjugation using the SpyTag-SpyCatcher system. When mice were i... More

關鍵詞

SARS-CoV-2; SpyTag-SpyCatcher; covalent conjugation; nanoparticles; receptor binding domain; vaccine.
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