| Literature DB >> 33232788 |
Diana Llopiz1, Marta Ruiz1, Leyre Silva1, David Repáraz1, Belén Aparicio1, Josune Egea1, Juan J Lasarte2, Esther Redin3, Alfonso Calvo3, Matthew Angel4, Jay A Berzofsky5, David Stroncek6, Pablo Sarobe7.
Abstract
Analyzing immunomodulatory elements operating during antitumor vaccination in prostate cancer patients and murine models we identified IL-10-producing DC as a subset with poorer immunogenicity and clinical efficacy. Inhibitory TAM receptors MER and AXL were upregulated on murine IL-10+ DC. Thus, we analyzed conditions inducing these molecules and the potential benefit of their blockade during vaccination. MER and AXL upregulation was more efficiently induced by a vaccine containing Imiquimod than by a poly(I:C)-containing vaccine. Interestingly, MER expression was found on monocyte-derived DC, and was dependent on IL-10. TAM blockade improved Imiquimod-induced DC activation in vitro and in vivo, resulting in increased vaccine-induced T-cell responses, which were further reinforced by concomitant IL-10 inhibition. In different tumor models, a triple therapy (including vaccination, TAM inhibition and IL-10 blockade) provided the strongest therapeutic effect, associated with enhanced T-cell immunity and enhanced CD8+ T cell tumor infiltration. Finally, MER levels in DC used for vaccination in cancer patients correlated with IL-10 expression, showing an inverse association with vaccine-induced clinical response. These results suggest that TAM receptors upregulated during vaccination may constitute an additional target in combinatorial therapeutic vaccination strategies.Entities:
Keywords: Dendritic cells; IL-10; MER; TAM receptors; Therapeutic vaccination
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Year: 2020 PMID: 33232788 PMCID: PMC8006848 DOI: 10.1016/j.canlet.2020.11.022
Source DB: PubMed Journal: Cancer Lett ISSN: 0304-3835 Impact factor: 8.679