Tumor associated antigens combined with carbon dots for inducing durable antitumor immunity.

[Display omitted] • CDs and CMs with good biocompatibility were prepared. • CMB and CMC stimulated the maturation of DC cells and activated T cells. • CMB and CMC can target LNs and induce an immune response to treat primary and distal tumor models. • CMB and CMC can specifically target B16F10 and CT26 tumors, respectively. Although therapeutic nanovaccines have made a mark in cancer immunotherapy, the shortcomings such as poor homing ability of lymph nodes (LNs), low antigen presentation efficiency and low antitumor efficacy have hindered their clinical transformation. Accordingly, we prepared advanced nanovaccines (CMB and CMC) by integrating carbon dots (CDs) with tumor-associated antigens (B16F10 and CT26). These nanovaccines could forwardly target tumors harbouring LNs, induce strong immunogenicity for activating cytotoxic T cells (CTLs), thereby readily eliminating tumor cells and suppressing primary/distal tumor growth. This work provides a promising therapeutic vaccination strategy to enhance cancer immunotherapy. [ABSTRACT FROM AUTHOR]