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Promoting antigen escape from dendritic cell endosomes potentiates anti-tumoral immunity

Jean‐Pierre Bikorimana, Natasha Salame, Simon Beaudoin, Mohammad Balood, Théo Crosson, Jamilah Abusarah, Sébastien Talbot, Raimar Löbenberg, Sebastien Plouffe, Moutih Rafei

2022Cell Reports Medicine31 citationsDOIOpen Access PDF

Abstract

The cross-presenting capacity of dendritic cells (DCs) can be limited by non-specific degradation during endosome maturation. To bypass this limitation, we present in this study a new Accum-based formulation designed to promote endosome-to-cytosol escape. Treatment of primary DCs with Accum linked to the xenoantigen ovalbumin (OVA) triggers endosomal damages and enhances protein processing. Despite multiple challenges using ascending doses of tumor cells, DC prophylactic vaccination results in complete protection due to increased levels of effector CD4 and CD8 T cells as well as high production of pro-inflammatory mediators. When combined with anti-PD-1, therapeutic vaccination using both syngeneic and allogeneic Accum-OVA-pulsed DCs triggers potent anti-tumoral responses. The net outcome culminates in increased CD11c, CD8, and NK infiltration along with a high CD8/Treg ratio. These highly favorable therapeutic effects highlight the promising potential of Accum as a distinct and potent technology platform suitable for the design of next generation cell cancer vaccines.

Topics & Concepts

EndosomeCross-presentationOvalbuminCD8CD11cDendritic cellCell biologyEffectorAntigenImmunologyVaccinationCytotoxic T cellImmune systemT cellBiologyCancer researchAntigen-presenting cellIntracellularPhenotypeBiochemistryGeneIn vitroImmunotherapy and Immune ResponsesRNA Interference and Gene DeliveryExtracellular vesicles in disease
Promoting antigen escape from dendritic cell endosomes potentiates anti-tumoral immunity | Litcius