Peptide–TLR-7/8a conjugate vaccines chemically programmed for nanoparticle self-assembly enhance CD8 T-cell immunity to tumor antigens

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Lynn, Geoffrey | Sedlik, Christine | Baharom, Faezzah | Zhu, Yaling | Ramirez-Valdez, Ramiro | Coble, Vincent | Tobin, Kennedy | Nichols, Sarah | Itzkowitz, Yaakov | Zaidi, Neeha | Gammon, Joshua | Blobel, Nicolas | Denizeau, Jordan | de La Rochere, Philippe | Francica, Brian | Decker, Brennan | Maciejewski, Mateusz | Cheung, Justin | Yamane, Hidehiro | Smelkinson, Margery | Francica, Joseph | Laga, Richard | Bernstock, Joshua | Seymour, Leonard | Drake, Charles | Jewell, Christopher | Lantz, Olivier | Piaggio, Eliane | Ishizuka, Andrew | Seder, Robert

Edité par CCSD ; Nature Publishing Group -

International audience. Personalized cancer vaccines targeting patient-specific neoantigens are a promising cancer treatment modality; however, neoantigen physicochemical variability can present challenges to manufacturing personalized cancer vaccines in an optimal format for inducing anticancer T cells. Here, we developed a vaccine platform (SNP-7/8a) based on charge-modified peptide-TLR-7/8a conjugates that are chemically programmed to self-assemble into nanoparticles of uniform size (~20 nm) irrespective of the peptide antigen composition. This approach provided precise loading of diverse peptide neoantigens linked to TLR-7/8a (adjuvant) in nanoparticles, which increased uptake by and activation of antigen-presenting cells that promote T-cell immunity. Vaccination of mice with SNP-7/8a using predicted neoantigens (n = 179) from three tumor models induced CD8 T cells against ~50% of neoantigens with high predicted MHC-I binding affinity and led to enhanced tumor clearance. SNP-7/8a delivering in silico-designed mock neoantigens also induced CD8 T cells in nonhuman primates. Altogether, SNP-7/8a is a generalizable approach for codelivering peptide antigens and adjuvants in nanoparticles for inducing anticancer T-cell immunity.

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