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   Direct Type I IFN but Not MDA5/TLR3 Activation of Dendritic Cells Is Required for Maturation and Metabolic Shift to Glycolysis after Poly IC Stimulation  
   
نویسنده pantel a. ,teixeira a. ,haddad e. ,wood e.g. ,steinman r.m. ,longhi m.p.
منبع plos biology - 2014 - دوره : 12 - شماره : 1
چکیده    Type i interferons (ifns) play an important role in direct antiviral defense as well as linking the innate and adaptive immune responses. on dendritic cells (dcs),ifns facilitate their activation and contribute to cd8+ and cd4+ t cell priming. however,the precise molecular mechanism by which ifns regulate maturation and immunogenicity of dcs in vivo has not been studied in depth. here we show that,after in vivo stimulation with the tlr ligand poly ic,ifns dominate transcriptional changes in dcs. in contrast to direct tlr3/mda5 signaling,ifns are required for upregulation of all pathways associated with dc immunogenicity. in addition,metabolic pathways,particularly the switch from oxidative phosphorylation to glycolysis,are also regulated by ifns and required for dc maturation. these data provide evidence for a metabolic reprogramming concomitant with dc maturation and offer a novel mechanism by which ifns modulate dc maturation. © 2014 pantel et al.
آدرس laboratory of cellular physiology and immunology,christopher h. browne center for immunology and immune diseases,the rockefeller university,new york,ny, United States, laboratory of cellular physiology and immunology,christopher h. browne center for immunology and immune diseases,the rockefeller university,new york,ny, United States, vaccine and gene therapy institute of florida,port st. lucie,fl, United States, william harvey research institute,barts and the london school of medicine and dentistry,queen mary,university of london,london, United Kingdom, laboratory of cellular physiology and immunology,christopher h. browne center for immunology and immune diseases,the rockefeller university,new york,ny, United States, laboratory of cellular physiology and immunology,christopher h. browne center for immunology and immune diseases,the rockefeller university,new york,ny,united states,william harvey research institute,barts and the london school of medicine and dentistry,queen mary,university of london,london, United Kingdom
 
     
   
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