先天免疫系统                        
                
                                
                        
                            小RNA                        
                
                                
                        
                            微泡                        
                
                                
                        
                            免疫系统                        
                
                                
                        
                            生物                        
                
                                
                        
                            基因沉默                        
                
                                
                        
                            病毒                        
                
                                
                        
                            免疫学                        
                
                                
                        
                            TLR9型                        
                
                                
                        
                            病毒复制                        
                
                                
                        
                            单核细胞                        
                
                                
                        
                            免疫                        
                
                                
                        
                            癌症研究                        
                
                                
                        
                            病毒学                        
                
                                
                        
                            基因                        
                
                                
                        
                            基因表达                        
                
                                
                        
                            DNA甲基化                        
                
                                
                        
                            遗传学                        
                
                        
                    
            作者
            
                Xin Chen,Liwen Wang,Qian Cheng,Zuqun Deng,Yishu Tang,Yuhan Yan,Luke Xie,Xin Li            
         
                    
        
    
            
            标识
            
                                    DOI:10.1016/j.bbadis.2024.167457
                                    
                                
                                 
         
        
                
            摘要
            
            DNA virus infection is a significant cause of morbidity and mortality in patients with multiple myeloma (MM). Monocyte dysfunction in MM patients plays a central role in infectious complications, but the precise molecular mechanism underlying the reduced resistance of monocytes to viruses in MM patients remains to be elucidated. Here, we found that MM cells were able to transfer microRNAs (miRNAs) to host monocytes/macrophages via MM cell-derived exosomes, resulting in the inhibition of innate antiviral immune responses. The screening of miRNAs enriched in exosomes derived from the bone marrow (BM) of MM patients revealed five miRNAs that negatively regulate the cGAS-STING antiviral immune response. Notably, silencing these miRNAs with antagomiRs in MM-bearing C57BL/KaLwRijHsd mice markedly reduced viral replication. These findings identify a novel mechanism whereby MM cells possess the capacity to inhibit the innate immune response of the host, thereby rendering patients susceptible to viral infection. Consequently, targeting the aberrant expression patterns of characteristic miRNAs in MM patients is a promising avenue for therapeutic intervention. Considering the miRNA score and relevant clinical factors, we formulated a practical and efficient model for the optimal assessment of susceptibility to DNA viral infection in patients with MM.
         
            
 
                 
                
                    
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