| Literature DB >> 33763654 |
Weldy V Bonilla1, Nicole Kirchhammer1, Anna-Friederike Marx1, Sandra M Kallert1, Magdalena A Krzyzaniak1, Min Lu1, Stéphanie Darbre2, Sarah Schmidt3, Josipa Raguz3, Ursula Berka3, Ilena Vincenti2, Mindaugas Pauzuolis2, Romy Kerber4, Sabine Hoepner5, Stephan Günther4, Carsten Magnus6, Doron Merkler2,7, Klaus K Orlinger3, Alfred Zippelius1,8, Daniel D Pinschewer1.
Abstract
Therapeutic vaccination regimens inducing clinically effective tumor-specific CD8+ T lymphocyte (CTL) responses are an unmet medical need. We engineer two distantly related arenaviruses, Pichinde virus and lymphocytic choriomeningitis virus, for therapeutic cancer vaccination. In mice, life-replicating vector formats of these two viruses delivering a self-antigen in a heterologous prime-boost regimen induce tumor-specific CTL responses up to 50% of the circulating CD8 T cell pool. This CTL attack eliminates established solid tumors in a significant proportion of animals, accompanied by protection against tumor rechallenge. The magnitude of CTL responses is alarmin driven and requires combining two genealogically distantly related arenaviruses. Vector-neutralizing antibodies do not inhibit booster immunizations by the same vector or by closely related vectors. Rather, CTL immunodominance hierarchies favor vector backbone-targeted responses at the expense of self-reactive CTLs. These findings establish an arenavirus-based immunotherapy regimen that allows reshuffling of immunodominance hierarchies and breaking self-directed tolerance for efficient tumor control.Entities:
Keywords: CD8 T cells; Pichinde virus; anti-vector immunity; arenavirus; lymphocytic choriomeningitis virus; pre-existing immunity; therapeutic tumor vaccine; tumor control; viral genealogy
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Year: 2021 PMID: 33763654 PMCID: PMC7974551 DOI: 10.1016/j.xcrm.2021.100209
Source DB: PubMed Journal: Cell Rep Med ISSN: 2666-3791