Analysis of tumor-infiltrating NK and T cells highlights IL-15 stimulation and TIGIT blockade as a combination immunotherapy strategy for soft tissue sarcomas

Judge, Sean J; Darrow, Morgan A.; Thorpe, Steve W; Gingrich, Alicia A.; O’Donnell, Edmond F.; Bellini, Alyssa; Sturgill, Ian R.; Vick, Logan V.; Dunai, Cordelia; Stoffel, Karl; Yue, Lyu; Chen, Shuai; Cho, May; Rebhun, Robert B.; Monjazeb, Arta M.; Murphy, William J.; Canter, Robert J.

doi:10.1136/jitc-2020-001355

Cited by 65 publications

(80 citation statements)

References 52 publications

(53 reference statements)

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“…Hence, detailed analyses would be truly beneficial in STSs. While intratumoral NK cells of STSs exhibit numerous activation and exhaustion markers, peripheral NK cells in STS patients were observed as functionally impaired [86,87]. Patients undergoing NK-cell based immunotherapies mostly profit from administration of IL-15, a potent NK cell activator, while anti-NKG2A therapy is still lacking among clinical trials in STSs [125,126].…”

Section: Discussionmentioning

confidence: 99%

“…Judge et al further demonstrated that intratumoral NK cells express more activation and exhaustion markers as compared to peripheral blood NK cells [87]. Furthermore, ex vivo stimulation with IL-15 further increased both activation and exhaustion markers in intratumoral and peripheral blood NK cells [87]. The authors observed a significant upregulation of TIGIT receptor and, therefore, suggested a therapeutic potential of TIGIT blockade together with IL-15 therapy [87].…”

Section: Natural Killer (Nk) Cell Infiltrationmentioning

confidence: 98%

“…Bücklein et al have provided a detailed analysis of NK cell presence and function in STSs patients and, unlike in other malignancies, peripheral blood NK cells exhibited a profound impairment in cell function, especially in the intermediate and high-grade STSs [86]. Judge et al further demonstrated that intratumoral NK cells express more activation and exhaustion markers as compared to peripheral blood NK cells [87]. Furthermore, ex vivo stimulation with IL-15 further increased both activation and exhaustion markers in intratumoral and peripheral blood NK cells [87].…”

Section: Natural Killer (Nk) Cell Infiltrationmentioning

confidence: 99%

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Novel Insights into the Immunotherapy of Soft Tissue Sarcomas: Do We Need a Change of Perspective?

et al. 2021

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Soft tissue sarcomas (STSs) are rare mesenchymal tumors. With more than 80 histological subtypes of STSs, data regarding novel biomarkers of strong prognostic and therapeutic value are very limited. To date, the most important prognostic factor is the tumor grade, and approximately 50% of patients that are diagnosed with high-grade STSs die of metastatic disease within five years. Systemic chemotherapy represents the mainstay of metastatic STSs treatment for decades but induces response in only 15–35% of the patients, irrespective of the histological subtype. In the era of immunotherapy, deciphering the immune cell signatures within the STSs tumors may discriminate immunotherapy responders from non-responders and different immunotherapeutic approaches could be combined based on the predominant cell subpopulations infiltrating the STS tumors. Furthermore, understanding the immune diversity of the STS tumor microenvironment (TME) in different histological subtypes may provide a rationale for stratifying patients according to the TME immune parameters. In this review, we introduce the most important immune cell types infiltrating the STSs tumors and discuss different immunotherapies, as well as promising clinical trials, that would target these immune cells to enhance the antitumor immune responses and improve the prognosis of metastatic STSs patients.

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Section: Discussionmentioning

confidence: 99%

Section: Natural Killer (Nk) Cell Infiltrationmentioning

confidence: 98%

Section: Natural Killer (Nk) Cell Infiltrationmentioning

confidence: 99%

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Novel Insights into the Immunotherapy of Soft Tissue Sarcomas: Do We Need a Change of Perspective?

et al. 2021

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“…Importantly, the therapeutic effect of TIGIT antibody blockade was found to be NK cell-dependent as antibody-mediated NK cell depletion in mice 24 h prior to TIGIT blockade abrogated the positive effects of TIGIT antibody treatment [ 104 ]. Similar studies in human peripheral blood NK cells showed that TIGIT blockade enhanced their anti-tumor activity against soft-tissue sarcoma and ovarian carcinoma tumor targets in vitro, and significantly, reduced tumor burden of mice with ovarian carcinoma xenografts [ 105 , 106 ]. These encouraging pre-clinical results have led to the initiation of multiple clinical trials using monoclonal anti-TIGIT antibodies alone or in combination with other checkpoint inhibitors (NCT02913313, NCT04570839].…”

Section: Strategies To Overcome the Tumor Microenvironmentmentioning

confidence: 94%

Design and Implementation of NK Cell-Based Immunotherapy to Overcome the Solid Tumor Microenvironment

Navin

Lam

Parihar

2020

Cancers

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Natural killer (NK) cells are innate immune effectors capable of broad cytotoxicity via germline-encoded receptors and can have conferred cytotoxic potential via the addition of chimeric antigen receptors. Combined with their reduced risk of graft-versus-host disease (GvHD) and cytokine release syndrome (CRS), NK cells are an attractive therapeutic platform. While significant progress has been made in treating hematological malignancies, challenges remain in using NK cell-based therapy to combat solid tumors due to their immunosuppressive tumor microenvironments (TMEs). The development of novel strategies enabling NK cells to resist the deleterious effects of the TME is critical to their therapeutic success against solid tumors. In this review, we discuss strategies that apply various genetic and non-genetic engineering approaches to enhance receptor-mediated NK cell cytotoxicity, improve NK cell resistance to TME effects, and enhance persistence in the TME. The successful design and application of these strategies will ultimately lead to more efficacious NK cell therapies to treat patients with solid tumors. This review outlines the mechanisms by which TME components suppress the anti-tumor activity of endogenous and adoptively transferred NK cells while also describing various approaches whose implementation in NK cells may lead to a more robust therapeutic platform against solid tumors.

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“…RLI also enhanced the anti-tumor activity of PD-1 antagonist [ 98 ]. TIGIT has emerged as an additional checkpoint inhibitor for novel combinatorial therapy with IL-15 [ 99 ].…”

Section: Il-15 In Combination Therapy For Cancermentioning

confidence: 99%

Heterodimeric IL-15 in Cancer Immunotherapy

Bergamaschi

Stravokefalou

Stellas

et al. 2021

Cancers

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Immunotherapy has emerged as a valuable strategy for the treatment of many cancer types. Interleukin-15 (IL-15) promotes the growth and function of cytotoxic CD8+ T and natural killer (NK) cells. It also enhances leukocyte trafficking and stimulates tumor-infiltrating lymphocytes expansion and activity. Bioactive IL-15 is produced in the body as a heterodimeric cytokine, comprising the IL-15 and the so-called IL-15 receptor alpha chain that are together termed “heterodimeric IL-15” (hetIL-15). hetIL-15, closely resembling the natural form of the cytokine produced in vivo, and IL-15:IL-15Rα complex variants, such as hetIL-15Fc, N-803 and RLI, are the currently available IL-15 agents. These molecules have showed favorable pharmacokinetics and biological function in vivo in comparison to single-chain recombinant IL-15. Preclinical animal studies have supported their anti-tumor activity, suggesting IL-15 as a general method to convert “cold” tumors into “hot”, by promoting tumor lymphocyte infiltration. In clinical trials, IL-15-based therapies are overall well-tolerated and result in the expansion and activation of NK and memory CD8+ T cells. Combinations with other immunotherapies are being investigated to improve the anti-tumor efficacy of IL-15 agents in the clinic.

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Analysis of tumor-infiltrating NK and T cells highlights IL-15 stimulation and TIGIT blockade as a combination immunotherapy strategy for soft tissue sarcomas

Cited by 65 publications

References 52 publications

Novel Insights into the Immunotherapy of Soft Tissue Sarcomas: Do We Need a Change of Perspective?

Novel Insights into the Immunotherapy of Soft Tissue Sarcomas: Do We Need a Change of Perspective?

Design and Implementation of NK Cell-Based Immunotherapy to Overcome the Solid Tumor Microenvironment

Heterodimeric IL-15 in Cancer Immunotherapy

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