Endometrial Tumor Microenvironment Alters Human NK Cell Recruitment, and Resident NK Cell Phenotype and Function

Degos, Clara; Heinemann, Mellie; Barrou, Julien; Boucherit, Nicolas; Lambaudie, Éric; Savina, Ariel; Gorvel, Laurent; Olive, Daniel

doi:10.3389/fimmu.2019.00877

Cited by 88 publications

(97 citation statements)

References 57 publications

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“…Moreover, a strong correlation has been observed between TIGIT expression on peripheral blood CD8 + T cells and AML relapse post‐transplantation . In endometrial cancer, high levels of TIGIT on tumour‐resident NK cells have been associated with disease severity . Finally, a high TIGIT/DNAM‐1 ratio on tumour‐infiltrating T regs was shown to correlate with poor clinical outcome following ICB targeting PD‐1 and/or CTLA‐4 .…”

Section: Tigit Inhibits Anti‐cancer Immune Responsesmentioning

confidence: 99%

“…TIGIT up‐regulation has been observed in various malignancies, including melanoma, breast cancer, non‐small‐cell lung carcinoma (NSCLC), colon adenocarcinoma (COAD), gastric cancer, acute myeloid leukaemia (AML) and multiple myeloma (MM) . Many studies reported up‐regulated TIGIT expression on CD8 + T cells, but there are also descriptions of increased TIGIT levels on tumour‐infiltrating T regs and NK cells . In mouse pre‐clinical models and in cancer patients, TIGIT expression on tumour‐infiltrating CD8 + T cells often correlates with increased expression of other inhibitory receptors such as PD‐1, lymphocyte‐activation gene 3 (LAG‐3), T‐cell immunoglobulin and mucin‐domain containing‐3 (TIM‐3), and with decreased expression of DNAM‐1 .…”

Section: Tigit Inhibits Anti‐cancer Immune Responsesmentioning

confidence: 99%

“…In particular, TIGIT expression on CD8 + T cells in the peripheral blood of gastric cancer patients has been associated with decreased cellular metabolism which resulted in impaired proliferation, cytokine production and migration . Similar to TIGIT + CD8 + T cells, TIGIT + NK cells infiltrating mouse subcutaneous tumours or human endometrial cancers were found to co‐express other inhibitory receptors, such as LAG‐3 and TIM‐3 .…”

Section: Tigit Inhibits Anti‐cancer Immune Responsesmentioning

confidence: 99%

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TIGIT as an emerging immune checkpoint

Harjunpää

Guillerey

2019

Clinical and Experimental Immunology

364

311

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T cell immunoglobulin and ITIM domain (TIGIT) is an inhibitory receptor expressed on lymphocytes that was recently propelled under the spotlight as a major emerging target in cancer immunotherapy. TIGIT interacts with CD155 expressed on antigen-presenting cells or tumour cells to downregulate T cell and natural killer (NK) cell functions. TIGIT has emerged as a key inhibitor of anti-tumour responses that can hinder multiple steps of the cancer immunity cycle. Pre-clinical studies indicated that TIGIT blockade may protect against various solid and haematological cancers. Several monoclonal antibodies (mAbs) that block the inhibitory activity of human TIGIT have been developed. Clinical trials are ongoing, investigating TIGIT blockade as a monotherapy or in combination with anti-PD1/PD-L1 mAbs for the treatment of patients with advanced solid malignancies. In this review, we cover our current knowledge on TIGIT, from its discovery in 2009 to its current status as a clinical target.

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Section: Tigit Inhibits Anti‐cancer Immune Responsesmentioning

confidence: 99%

Section: Tigit Inhibits Anti‐cancer Immune Responsesmentioning

confidence: 99%

Section: Tigit Inhibits Anti‐cancer Immune Responsesmentioning

confidence: 99%

See 1 more Smart Citation

TIGIT as an emerging immune checkpoint

Harjunpää

Guillerey

2019

Clinical and Experimental Immunology

364

311

View full text Add to dashboard Cite

show abstract

“…Here, as well, blocking TIM-3 with antibodies increased NK cell cytotoxicity and cytokine secretion. Additional recent studies identified TIM-3 expression as a marker of NK cell dysfunction and disease severity in colorectal cancer, esophageal cancer, endometrial cancer, and bladder cancer (96,(98)(99)(100)(101). Interestingly, TIM-3 engagement was initially shown to increase the expression of IFN-γ by NK cells in response to galectin-9, the β-galactoside binding lectin (123).…”

Section: Tim-3mentioning

confidence: 99%

Unleashing Natural Killer Cells in the Tumor Microenvironment–The Next Generation of Immunotherapy?

2020

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The emergence of immunotherapy for cancer treatment bears considerable clinical promise. Nevertheless, many patients remain unresponsive, acquire resistance, or suffer dose-limiting toxicities. Immune-editing of tumors assists their escape from the immune system, and the tumor microenvironment (TME) induces immune suppression through multiple mechanisms. Immunotherapy aims to bolster the activity of immune cells against cancer by targeting these suppressive immunomodulatory processes. Natural Killer (NK) cells are a heterogeneous subset of immune cells, which express a diverse array of activating and inhibitory germline-encoded receptors, and are thus capable of directly targeting and killing cancer cells without the need for MHC specificity. Furthermore, they play a critical role in triggering the adaptive immune response. Enhancing the function of NK cells in the context of cancer is therefore a promising avenue for immunotherapy. Different NK-based therapies have been evaluated in clinical trials, and some have demonstrated clinical benefits, especially in the context of hematological malignancies. Solid tumors remain much more difficult to treat, and the time point and means of intervention of current NK-based treatments still require optimization to achieve long term effects. Here, we review recently described mechanisms of cancer evasion from NK cell immune surveillance, and the therapeutic approaches that aim to potentiate NK function. Specific focus is placed on the use of specialized monoclonal antibodies against moieties on the cancer cell, or on both the tumor and the NK cell. In addition, we highlight newly identified mechanisms that inhibit NK cell activity in the TME, and describe how biochemical modifications of the TME can synergize with current treatments and increase susceptibility to NK cell activity.

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“…CXCL9 and CXCL10 are binding to CXC-chemokine receptor 3 on effector CD8 + T cells, T H 1 cells, and NK cells, thereby regulating their recruitment into tumors (Nagarsheth et al 2017). CXCL10, which is an important factor in NK cell-recruitment and NK cell-mediated lysis of tumor cells has been shown to be strongly produced in the tumor compared to the adjacent tissue, suggesting that an immune response is occurring in the tumor (Degos et al 2019). In various malignancies, CXCL9 and CXCL10 were reported to be produced predominantly by activated CD103 + dendritic cells, (tumor-associated) macrophages and tumor cells (Lieber et al 2018;Spranger et al 2017).…”

Section: Role Of Chemokines In Tumor Immunology and In Immunotherapymentioning

confidence: 99%

Serum Chemokine-release Profiles in AML-patients Might Contribute to Predict the Clinical Course of the Disease

Merle

Fischbacher

Liepert

et al. 2019

Immunological Investigations

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In cancer or hematologic disorders, chemokines act as growth-or survival factors, regulating hematopoiesis and angiogenesis, determining metastatic spread and controlling leukocyte infiltration into tumors to inhibit antitumor immune responses. The aim was to quantify the release of CXCL8, −9, −10, CCL2, −5, and IL-12 in AML/ MDS-pts' serum by cytometric bead array and to correlate data with clinical subtypes and courses. Minimal differences in serum-levels subdivided into various groups (e.g. age groups, FAB-types, blastproportions, cytogenetic-risk-groups) were seen, but higher release of CXCL8, −9, −10 and lower release of CCL2 and −5 tendentially correlated with more favorable subtypes (<50 years of age, <80% blasts in PB). Comparing different stages of the disease higher CCL5-release in persisting disease and a significantly higher CCL2release at relapse were found compared to first diagnosispointing to a change of 'disease activity' on a chemokine level. Correlations with later on achieved response to immunotherapy and occurrence of GVHD were seen: Higher values of CXCL8, −9, −10 and CCL2 and lower CCL5-values correlated with achieved response to immunotherapy. Predictive cut-off-values were evaluated separating the groups in 'responders' and 'non-responders'. Higher levels of CCL2 and −5 but lower levels of CXCL8, −9, −10 correlated with occurrence of GVHD. We conclude, that in AML-pts' serum higher values of CXCL8, −9, −10 and lower values of CCL5 and in part of CCL2 correlate with more favorable subtypes and improved antitumor'-reactive function. This knowledge can contribute to develop immune-modifying strategies that promote antileukemic adaptive immune responses.

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Endometrial Tumor Microenvironment Alters Human NK Cell Recruitment, and Resident NK Cell Phenotype and Function

Cited by 88 publications

References 57 publications

TIGIT as an emerging immune checkpoint

TIGIT as an emerging immune checkpoint

Unleashing Natural Killer Cells in the Tumor Microenvironment–The Next Generation of Immunotherapy?

Serum Chemokine-release Profiles in AML-patients Might Contribute to Predict the Clinical Course of the Disease

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