Glycan-costumed virus-like particles promote type 1 anti-tumor immunity

Author:

Lensch ValerieORCID,Gabba AdeleORCID,Hincapie RobertORCID,Bhagchandani Sachin H.ORCID,Basak AnkitORCID,Alam Mohammad MurshidORCID,Irvine Darrell J.ORCID,Shalek Alex K.ORCID,Johnson Jeremiah A.ORCID,Finn M. G.ORCID,Kiessling Laura L.ORCID

Abstract

AbstractCancer vaccine development is inhibited by a lack of strategies for directing dendritic cell (DC) induction of effective tumor-specific cellular immunity. Pathogen engagement of DC lectins and toll-like receptors (TLRs) shapes immunity by directing T cell function. Strategies to activate specific DC signaling pathways via targeted receptor engagement are crucial to unlocking type 1 cellular immunity. Here, we engineered a glycan-costumed virus-like particle (VLP) vaccine that delivers programmable peptide antigens to induce tumor-specific cellular immunityin vivo. VLPs encapsulating TLR7 agonists and decorated with a selective mannose-derived ligand for the lectin DC-SIGN induced robust DC activation and type 1 cellular immunity, whereas VLPs lacking this key DC-SIGN ligand failed to promote DC-mediated immunity. Vaccination with glycan-costumed VLPs generated tumor antigen-specific Th1 CD4+and CD8+T cells that infiltrated solid tumors, inhibiting tumor growth in a murine melanoma model. Thus, VLPs employing lectin-driven immune reprogramming provide a framework for advancing cancer immunotherapies.

Publisher

Cold Spring Harbor Laboratory

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