IFN-III is selectively produced by cDC1 and predicts good clinical outcome in breast cancer
Author(s) -
Margaux Hubert,
Élisa Gobbini,
Coline Couillault,
ThienPhong Vu Manh,
AnneClaire Doffin,
Justine Berthet,
Céline Rodriguez,
Vincent Ollion,
Janice Kielbassa,
Christophe Sajous,
Isabelle Treilleux,
Olivier Trédan,
Bertrand Dubois,
Marc Dalod,
Nathalie BendrissVermare,
Christophe Caux,
Jenny ValladeauGuilemond
Publication year - 2020
Publication title -
science immunology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 8.83
H-Index - 51
ISSN - 2470-9468
DOI - 10.1126/sciimmunol.aav3942
Subject(s) - immune system , immunotherapy , cancer research , chemokine , tumor microenvironment , dendritic cell , ccr4 , biology , interferon , immunology , cytotoxic t cell , medicine , chemokine receptor , biochemistry , in vitro
Dendritic cells play a key role in the orchestration of antitumor immune responses. The cDC1 (conventional dendritic cell 1) subset has been shown to be essential for antitumor responses and response to immunotherapy, but its precise role in humans is largely unexplored. Using a multidisciplinary approach, we demonstrate that human cDC1 play an important role in the antitumor immune response through their capacity to produce type III interferon (IFN-λ). By analyzing a large cohort of breast primary tumors and public transcriptomic datasets, we observed specific production of IFN-λ1 by cDC1. In addition, both IFN-λ1 and its receptor were associated with favorable patient outcomes. We show that IFN-III promotes a T H 1 microenvironment through increased production of IL-12p70, IFN-γ, and cytotoxic lymphocyte-recruiting chemokines. Last, we showed that engagement of TLR3 is a therapeutic strategy to induce IFN-III production by tumor-associated cDC1. These data provide insight into potential IFN- or cDC1-targeting antitumor therapies.
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