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Tumor-targeted silencing of the peptide transporter TAP induces potent antitumor immunity

Nat Commun.. 2019; 
Garrido G1, Schrand B1, Rabasa A1, Levay A1, D'Eramo F1, Berezhnoy A1, Modi S2, Gefen T1, Marijt K3, Doorduijn E3, Dudeja V2, van Hall T3, Gilboa E4.
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摘要

Neoantigen burden is a major determinant of tumor immunogenicity, underscored by recent clinical experience with checkpoint blockade therapy. Yet the majority of patients do not express, or express too few, neoantigens, and hence are less responsive to immune therapy. Here we describe an approach whereby a common set of new antigens are induced in tumor cells in situ by transient downregulation of the transporter associated with antigen processing (TAP). Administration of TAP siRNA conjugated to a broad-range tumor-targeting nucleolin aptamer inhibited tumor growth in multiple tumor models without measurable toxicity, was comparatively effective to vaccination against prototypic mutation-generated neoantigens, ... More

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