Expansion and Activation of CD103+ Dendritic Cell Progenitors at the Tumor Site Enhances Tumor Responses to Therapeutic PD-L1 and BRAF Inhibition

Salmon, Hélène; Idoyaga, Juliana; Rahman, Adeeb; Leboeuf, Marylène; Remark, Romain; Jordan, Stefan; Casanova-Acebes, María; Khudoynazarova, Makhzuna; Agudo, Judith; Tung, Navpreet; Chakarov, Svetoslav; Rivera, Christina G.; Hogstad, Brandon; Bosenberg, Marcus W.; Hashimoto, Daigo; Gnjatic, Sacha; Bhardwaj, Nina; Palucka, A. Karolina; Brown, Brian D.; Brody, Joshua; Ginhoux, Florent; Mérad, Miriam

doi:10.1016/j.immuni.2016.03.012

Cited by 882 publications

(961 citation statements)

References 46 publications

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“…In the B-Raf/PTEN −/− / β-catenin genetically engineered mouse model, this has been pursued by generating bone marrow-derived DCs using Flt3L followed by activation with the TLR3 agonist poly I:C. Injection of these DCs directly into the tumor microenvironment restored T cell priming, effector T cell recruitment, and caused partial tumor shrinkage, which was amplified with co-administration of anti-CT-LA-4 and anti-PD-L1 mAbs [102]. In a related strategy, systemic administration of Flt3L to increase Batf3 DCs in the tumor microenvironment, combined with intratumoral injection of poly I:C had a similar effect [46]. These are approaches that are immediately testable in the clinic with available reagents.…”

Section: Therapeutic Opportunitiesmentioning

confidence: 96%

“…Type I IFNs are also expressed by leukocytes in the tumor and tumor-draining lymph node in an autochthonous melanoma model driven by melanocyte-specific activating mutation in BRAF and deletion of PTEN [45]. Recently, it was demonstrated that CD103 + DCs are uniquely capable of transporting tumor-derived antigens to the tumor-draining lymph node in a CCR7-dependent manner, where they prime antigen-specific CD8 + T cells [46]. This process was augmented in an IFNAR-dependent manner, revealed by a combination treatment of tumor-bearing mice with Fms-related tyrosine kinase 3 ligand (Flt3L) and intratumoral injection of polyinosinic:polycytidylic acid (poly I:C).…”

Section: The Central Role For Type I Ifns and Batf3 Dcsmentioning

confidence: 99%

“…This process was augmented in an IFNAR-dependent manner, revealed by a combination treatment of tumor-bearing mice with Fms-related tyrosine kinase 3 ligand (Flt3L) and intratumoral injection of polyinosinic:polycytidylic acid (poly I:C). The improvement of tumor control with this treatment was attributed to Flt3L-mediated expansion of the tumor-infiltrating CD103 + DCs and their activation by poly I:C via the toll-like receptor 3 (TLR3)-TIR-domain containing adapter-inducing IFN-β (TRIF) pathway [46]. Collectively, these findings support a model in which type I IFN production in the tumor facilitates antigen cross-presentation by Batf3 DCs, which then migrate via the lymphatics to the tumor-draining lymph nodes, where they cross-prime naive CD8 + T cells.…”

Section: The Central Role For Type I Ifns and Batf3 Dcsmentioning

confidence: 99%

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Innate immune signaling and regulation in cancer immunotherapy

et al. 2016

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A pre-existing T cell-inflamed tumor microenvironment has prognostic utility and also can be predictive for response to contemporary cancer immunotherapies. The generation of a spontaneous T cell response against tumor-associated antigens depends on innate immune activation, which drives type I interferon (IFN) production. Recent work has revealed a major role for the STING pathway of cytosolic DNA sensing in this process. This cascade of events contributes to the activation of Batf3-lineage dendritic cells (DCs), which appear to be central to anti-tumor immunity. Non-T cell-inflamed tumors lack chemokines for Batf3 DC recruitment, have few Batf3 DCs, and lack a type I IFN gene signature, suggesting that failed innate immune activation may be the ultimate cause for lack of spontaneous T cell activation and accumulation. With this information in hand, new strategies for triggering innate immune activation and Batf3 DC recruitment are being developed, including novel STING agonists for de novo immune priming. Ultimately, the successful development of effective innate immune activators should expand the fraction of patients that can respond to immunotherapies, such as with checkpoint blockade antibodies.

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Section: Therapeutic Opportunitiesmentioning

confidence: 96%

Section: The Central Role For Type I Ifns and Batf3 Dcsmentioning

confidence: 99%

Section: The Central Role For Type I Ifns and Batf3 Dcsmentioning

confidence: 99%

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Innate immune signaling and regulation in cancer immunotherapy

et al. 2016

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“…caused by chronic inflammation of synovial tissue. During the onset of RA, an acute inflammation of the synovial lining (synovitis) leads to an extensive expansion of the corresponding cells (i.e., pannus formation and inflammatory cytokines), massive infiltration of leukocytes of the innate immune system (i.e., T and B cells, plasmocytes, and macrophages), and synovial fibroblast proliferation (8)(9)(10). The latter are regarded as effector cells responsible for cartilage and bone destruction in RA.…”

Section: Discussionmentioning

confidence: 99%

TRAF6 regulates the effects of polarized maturation of tolerability: Marrow-derived dendritic cells on collagen-induced arthritis in mice

et al. 2017

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Abstract. The study aimed to investigate the re lationship between tumor necrosis factor receptor-associated factor 6 (TRAF6) and a differentially mature dendritic cell (mDC) in collagen-induced arthritis (CIA) mice and to determine whether or not TRAF6 regulates the activation of an immature dendritic cell (iDC) and inhibits iDC maturation to induce immune tolerance. The mouse bone marrow stem cells were induced with recombinant granulocyte-macrophage colony-stimulating factor (rmGM-CSF) and recombinant interleukin-4 (rmIL-4) to differentiate immature dendritic cells (DCs), which were divided into four groups with different maturation states: rmGM-CSF, rmIL-4; TNF-α; LPS; and FK506 group. The levels of the cell surfaces of CD80, CD86, and MHI-Ⅱ were analyzed by flow cytometry to prove DCs at different levels of maturity. The expression of IL-12 in DCs at different maturation states was detected by enzyme-linked immunosorbent assay (ELISA). The expression of TRAF6 mRNA and protein in each group of DCs was detected by a reverse transcription-polymerase chain reaction (RT-PCR) and western blot analysis. The results revealed that the differentiation of bone marrow cells into iDCs was significantly induced by cytokines (rmGM-CSF, IL-4). CD80, CD86, MHC-Ⅱ were expressed in the four groups, and the difference between them was statistically significant (P<0.05). A higher degree of DC differentiation led to a gradual increase of IL-12 secretion in the four groups. The difference was statistically significant (P<0.05) for this secretion (group D, 10,620.73±276.73 pg/ml). The exp ression levels of TRAF6 mRNA were significantly higher in group D than those in the other three groups (P<0.01). Although there was no significant difference in the expression levels of TRAF6 mRNA between groups B and C, the expression levels of TRAF6 mRNA between groups B and C were higher than those of the control group. The TRAF6 protein expression was higher in group D than that in the other three groups (P<0

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“…This may or may not be linked to the role of activated mononuclear phagocytes/macrophages in the outcome of checkpoint therapy [45] where it has been shown that the induction of the CD103 + marker on DCs is an absolute required for PD-1-based therapy to be effective in a murine model. This is of interest as a review of many different vaccine studies over the last two decades highlighted the excellent long-term outcome of patients given a heat-killed mycobacterium vaccine preparation (also known as SRL-172) with stage IV melanoma patients achieving similar 5-and 8-year survivals to that reported using ipilimumab.…”

Section: Novel Immunotherapeutics and Future Perspectivementioning

confidence: 99%

The importance for immunoregulation for long-term cancer control

Fusi

Dalgleish

2017

Future Oncology

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Immune checkpoint blockades have recently emerged as a breakthrough treatment for solid tumors showing high response rates and long durability. In melanoma, the combination of ipilimumab with nivolumab showed high efficacy. However, still half the patients do not respond to this treatment. In order to increase the therapeutic ratio in melanoma and other cancers, different approaches are under evaluation. Three relevant questions are at the moment driving the research community: how to maximize benefit while minimizing toxicity; how to better identify patients who are more likely to benefit from immunotherapy; how to convert nonresponders into responders. In this review we summarize the most recent findings and we outline the most likely future challenges.

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Expansion and Activation of CD103+ Dendritic Cell Progenitors at the Tumor Site Enhances Tumor Responses to Therapeutic PD-L1 and BRAF Inhibition

Cited by 882 publications

References 46 publications

Innate immune signaling and regulation in cancer immunotherapy

Innate immune signaling and regulation in cancer immunotherapy

TRAF6 regulates the effects of polarized maturation of tolerability: Marrow-derived dendritic cells on collagen-induced arthritis in mice

The importance for immunoregulation for long-term cancer control

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