| Literature DB >> 24589924 |
Tobias Bald1, Jennifer Landsberg1, Dorys Lopez-Ramos1, Marcel Renn1, Nicole Glodde1, Philipp Jansen1, Evelyn Gaffal1, Julia Steitz1, Rene Tolba1, Ulrich Kalinke1, Andreas Limmer1, Göran Jönsson1, Michael Hölzel1, Thomas Tüting2.
Abstract
UNLABELLED: Infiltration of human melanomas with cytotoxic immune cells correlates with spontaneous type I IFN activation and a favorable prognosis. Therapeutic blockade of immune-inhibitory receptors in patients with preexisting lymphocytic infiltrates prolongs survival, but new complementary strategies are needed to activate cellular antitumor immunity in immune cell-poor melanomas. Here, we show that primary melanomas in Hgf-Cdk4(R24C) mice, which imitate human immune cell-poor melanomas with a poor outcome, escape IFN-induced immune surveillance and editing. Peritumoral injections of immunostimulatory RNA initiated a cytotoxic inflammatory response in the tumor microenvironment and significantly impaired tumor growth. This critically required the coordinated induction of type I IFN responses by dendritic, myeloid, natural killer, and T cells. Importantly, antibody-mediated blockade of the IFN-induced immune-inhibitory interaction between PD-L1 and PD-1 receptors further prolonged the survival. These results highlight important interconnections between type I IFNs and immune-inhibitory receptors in melanoma pathogenesis, which serve as targets for combination immunotherapies. SIGNIFICANCE: Using a genetically engineered mouse melanoma model, we demonstrate that targeted activation of the type I IFN system with immunostimulatory RNA in combination with blockade of immune-inhibitory receptors is a rational strategy to expose immune cell-poor tumors to cellular immune surveillance. ©2014 American Association for Cancer Research.Entities:
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Year: 2014 PMID: 24589924 DOI: 10.1158/2159-8290.CD-13-0458
Source DB: PubMed Journal: Cancer Discov ISSN: 2159-8274 Impact factor: 39.397