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Enhanced Class I Tumor Antigen Presentation via Cytosolic Delivery of Exosomal Cargos by Tumor-Cell-Derived Exosomes Displaying a pH-Sensitive Fusogenic Peptide.

Mol. Pharm.. 2017; 
MorishitaMasaki,TakahashiYuki,NishikawaMakiya,AriizumiReiichi,TakakuraYoshi
Products/Services Used Details Operation
Catalog Peptides GALA (NH2−WEAALAEALAEALAEHLAEALAEALEALAA-COOH) modified with biotin−aminohexanoic acid (Ahx) at the N-terminus was purchased from GenScript (Piscataway, NJ, U.S.A.). GALA modified with biotin−Ahx at the N-terminus and fluorescein isothiocyanate (FITC) at the C-terminus was also purchased from GenScript and used to evaluate the modification efficiency of GALA on exosomes. Get A Quote

摘要

Tumor-cell-derived exosomes contain endogenous tumor antigens and can be used as a potential cancer vaccine without requiring identification of the tumor-specific antigen. To elicit an effective antitumor effect, efficient tumor antigen presentation by MHC class I molecules on dendritic cells (DC) is desirable. Because DC endocytose exosomes, an endosomal escape mechanism is required for efficient MHC class I presentation of exosomal tumor antigens. In the present study, efficient cytosolic delivery of exosomal tumor antigens was performed using genetically engineered tumor-cell-derived exosomes and pH-sensitive fusogenic GALA peptide. Murine melanoma B16BL6 cells were transfected with a plasmid vector en... More

关键词

GALA,MHC class I molecule,cytosolic delivery,exosome,tumor antigen presenta