TLR7型                        
                
                                
                        
                            免疫系统                        
                
                                
                        
                            浆细胞样树突状细胞                        
                
                                
                        
                            获得性免疫系统                        
                
                                
                        
                            免疫学                        
                
                                
                        
                            先天免疫系统                        
                
                                
                        
                            生物                        
                
                                
                        
                            癌症免疫疗法                        
                
                                
                        
                            肿瘤微环境                        
                
                                
                        
                            免疫疗法                        
                
                                
                        
                            干扰素                        
                
                                
                        
                            树突状细胞                        
                
                                
                        
                            Ⅰ型干扰素                        
                
                                
                        
                            癌症                        
                
                                
                        
                            抗原                        
                
                                
                        
                            免疫                        
                
                                
                        
                            Toll样受体                        
                
                                
                        
                            遗传学                        
                
                        
                    
            作者
            
                Dana K. Mitchell,Sreenivasulu Chintala,Mahua Dey            
         
                    
        
    
            
            标识
            
                                    DOI:10.1016/j.jneuroim.2018.06.012
                                    
                                
                                 
         
        
                
            摘要
            
            Plasmacytoid dendritic cells (pDCs) comprise a subset of dendritic cells characterized by their ability to produce large amount of type I interferon (IFN-I/α). Originally recognized for their role in modulating immune responses to viral stimulation, growing interest has been directed toward their contribution to tumorigenesis. Under normal conditions, Toll-like receptor (TLR)-activated pDCs exhibit robust IFN-α production and promote both innate and adaptive immune responses. In cancer, however, pDCs demonstrate an impaired response to TLR7/9 activation, decreased or absent IFN-α production and contribute to the establishment of an immunosuppressive tumor microenvironment. In addition to IFN-α production, pDCs can also act as antigen presenting cells (APCs) and regulate immune responses to various antigens. The significant role played by pDCs in regulating both the innate and adaptive components of the immune system makes them a critical player in cancer immunology. In this review, we discuss the development and function of pDCs as well as their role in innate and adaptive immunity. Finally, we summarize pDC contribution to cancer pathogenesis, with a special focus on primary malignant brain tumor, their significance in the era of immunotherapy and suggest potential strategies for pDC-targeted therapy.
         
            
 
                 
                
                    
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