衣壳                        
                
                                
                        
                            免疫原性                        
                
                                
                        
                            细胞生物学                        
                
                                
                        
                            折叠(DSP实现)                        
                
                                
                        
                            蛋白质折叠                        
                
                                
                        
                            化学                        
                
                                
                        
                            生物物理学                        
                
                                
                        
                            膜蛋白                        
                
                                
                        
                            生物                        
                
                                
                        
                            病毒学                        
                
                                
                        
                            计算生物学                        
                
                                
                        
                            膜                        
                
                                
                        
                            生物化学                        
                
                                
                        
                            病毒                        
                
                                
                        
                            遗传学                        
                
                                
                        
                            免疫系统                        
                
                                
                        
                            电气工程                        
                
                                
                        
                            工程类                        
                
                        
                    
            作者
            
                Junru Cui,Fangfeng Yuan,Jane Qin,Ju Hyeong Jeon,Dong Soo Yun,Tianlei Wang,Ren-Huan Xu,Hong Cao,Ashleigh A. Tungate,Christopher L. Netherton,Jianzhu Chen            
         
                    
        
    
            
            标识
            
                                    DOI:10.1021/acsinfecdis.5c00067
                                    
                                
                                 
         
        
                
            摘要
            
            Viral capsid proteins are widely explored for subunit vaccine development but are often hampered by their complexity of production and low immunogenicity. Here, we report a simple approach to overcoming these challenges by combining mRNA vaccine technology with protein engineering. Using African swine fever virus (ASFV) capsid proteins P72 and penton as models, we engineered them into membrane-bound and secreted forms and compared their immunogenicity to that of the native intracellular form in mice and pigs through mRNA vaccination. The membrane-bound and secreted P72 and penton folded into their native multimeric structure independent of the viral chaperone, therefore preserving their conformational epitopes. The membrane-bound P72 and penton also elicited significantly stronger antibody and T cell responses than their secreted or intracellular counterparts. Our study provides a simple approach to enhancing folding, multimeric structure formation, and immunogenicity of viral capsid proteins for ASFV subunit vaccine development and immunogenicity of intracellular proteins in general.
         
            
 
                 
                
                    
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