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Antigen-loaded monocyte administration induces potent therapeutic antitumor T cell responses.

J Clin Invest. 2020; 
Huang MN,, Nicholson LT, Batich KA,,, Swartz AM,, Kopin D, Wellford S, Prabhakar VK, Woroniecka K,,, Nair SK,,,, Fecci PE,,, Sampson JH,,, Gunn MD,.
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Catalog Peptides (both at 250 μg/mL; AnaSpec), or 5-carboxyfluorescein– labeled (FAM-labeled) SIINFEKL (10–500 μg/mL; GenScript) in cRPMI-20 medium for 2 hours with 5% CO2 at 37°C. For PTX (MilliporeSigma) Get A Quote

摘要

Efficacy of dendritic cell (DC) cancer vaccines is classically thought to depend on their antigen-presenting cell (APC) activity. Studies show, however, that DC vaccine priming of cytotoxic T lymphocytes (CTLs) requires the activity of endogenous DCs, suggesting that exogenous DCs stimulate antitumor immunity by transferring antigens (Ags) to endogenous DCs. Such Ag transfer functions are most commonly ascribed to monocytes, implying that undifferentiated monocytes would function equally well as a vaccine modality and need not be differentiated to DCs to be effective. Here, we used several murine cancer models to test the antitumor efficacy of undifferentiated monocytes loaded with protein or peptide Ag. Intrav... More

关键词

Cancer immunotherapy; Dendritic cells; Immunology; Monocytes; Vaccines