Targeting Treg cells in cancer immunotherapy

Tanaka, Atsushi; Sakaguchi, Shimon

doi:10.1002/eji.201847659

Cited by 318 publications

(209 citation statements)

References 60 publications

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“…Increased pro-inflammatory chemokines Immune system modulation (Tokunaga et,al., 2018) 9 Increased Tregs Immune system modulation (Tanaka and,Sakaguchi, 2019) 10 Kyurenine signature Targeted inhibition and immune modulation (Labadie et al, 2019) (Chomienne et al, 1990). If deployed at the appropriate time, treatments that target liabilities of a specific cell state or prevent further adaptation may help improve patient survival by constraining continued tumor evolution towards complete drug resistance.…”

Section: R a F Tmentioning

confidence: 99%

Heterogeneity and targeted therapy-induced adaptations in lung cancer revealed by longitudinal single-cell RNA sequencing

Maynard

McCoach

Rotow

et al. 2019

Preprint

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Section: R a F Tmentioning

confidence: 99%

Heterogeneity and targeted therapy-induced adaptations in lung cancer revealed by longitudinal single-cell RNA sequencing

Maynard

McCoach

Rotow

et al. 2019

Preprint

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“…Notably, because of their ability to directly kill tumor cells and a better knowledge of MHC class I tumor antigens, much more attention has been dedicated to the role of CD8 + T cells (37)(38)(39). In the meantime, many studies have also elucidated the detrimental role of CD4 + Treg cells in antitumor immunity and put these cells at the center stage as immunotherapy targets (40). Our work brings to light that consistently large fractions of total T cells infiltrating the tumor are made up of non-Treg CD4 + T cells in both colorectal and lung cancer.…”

Section: Discussionmentioning

confidence: 74%

Bystander CD4⁺T cells infiltrate human tumors and are phenotypically distinct

Simoni

Zhuang

et al. 2020

Preprint

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Tumor-specific T cells likely underpin effective immune checkpoint-blockade therapies. Yet, most studies focus on Treg cells and CD8+ tumor-infiltrating lymphocytes (TILs). Here we study CD4+ TILs in human lung and colorectal cancers and observe that non-Treg CD4+ TILs average more than 70% of total CD4+ TILs in both cancer types. Leveraging high dimensional analyses including mass cytometry and single-cell sequencing, we reveal that CD4+ TILs are heterogeneous at both gene and protein levels, within each tumor and across patients. Consistently, we find different subsets of CD4+ TILs showing characteristics of effectors, tissue resident memory (Trm) or exhausted cells (expressing PD-1, CTLA-4 and CD39). In both cancer types, the frequencies of CD39− non-Treg CD4+ TILs strongly correlate with frequencies of CD39− CD8+ TILs, which we and others have previously shown to be enriched for cells specific for cancer-unrelated antigens (bystanders). Ex-vivo, we demonstrate that CD39− CD4+ TILs can be specific for cancer unrelated antigens, such as HCMV epitopes. Overall, our findings highlight that CD4+ TILs cells are not necessarily tumor-specific and suggest measuring CD39 expression as a straightforward way to quantify or isolate bystander CD4+ T cells.Graphical abstract

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“…As ICIs have not generally been successful on their own due to a number of immunological and physiological challenges, combination treatments that perturb the TIME from cold to hot are appealing . The advantage of taPIT over conventional modalities is the potential to more precisely modulate the TIME through specific targeting of cancer and immunosuppressive tumor cell subtypes including tumor‐associated macrophages , fibroblasts and regulatory T cells . Although the in vitro model in this work overestimates clinical measurements of E:T ratios in ovarian cancer , sparing local cytotoxic T cells may prove critical in future taPIT–ICI treatment strategies that facilitate a robust immune response after photodynamic destruction.…”

Section: Resultsmentioning

confidence: 98%

Section: Resultsmentioning

confidence: 99%

Cancer Cell‐targeted and Activatable Photoimmunotherapy Spares T Cells in a 3D Coculture Model

Kercher

Nath

Rizvi

et al. 2019

Photochem & Photobiology

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Photodynamic therapy (PDT) is an established therapeutic modality that uses nonionizing near‐infrared light to activate photocytotoxicity of endogenous or exogenous photosensitizers (PSs). An ongoing avenue of cancer research involves leveraging PDT to stimulate antitumor immune responses; however, these effects appear to be best elicited in low‐dose regimens that do not provide significant tumor reduction using conventional, nonspecific PSs. The loss of immune enhancement at higher PDT doses may arise in part from indiscriminate damage to local immune cell populations, including tumor‐infiltrating T cells. We previously introduced “tumor‐targeted, activatable photoimmunotherapy” (taPIT) using molecular‐targeted and cell‐activatable antibody–PS conjugates to realize precision tumor photodamage with microscale fidelity. Here, we investigate the immune cell sparing effect provided by taPIT in a 3D model of the tumor immune microenvironment. We report that high‐dose taPIT spares 25% of the local immune cell population, five times more than the conventional PDT regimen, in a 3D coculture model incorporating epithelial ovarian cancer cells and T cells. These findings suggest that the enhanced selectivity of taPIT may be utilized to achieve local tumor reduction with sparing of intratumor effector immune cells that would otherwise be lost if treated with conventional PDT.

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Targeting Treg cells in cancer immunotherapy

Cited by 318 publications

References 60 publications

Heterogeneity and targeted therapy-induced adaptations in lung cancer revealed by longitudinal single-cell RNA sequencing

Heterogeneity and targeted therapy-induced adaptations in lung cancer revealed by longitudinal single-cell RNA sequencing

Bystander CD4⁺T cells infiltrate human tumors and are phenotypically distinct

Cancer Cell‐targeted and Activatable Photoimmunotherapy Spares T Cells in a 3D Coculture Model

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Targeting Treg cells in cancer immunotherapy

Cited by 318 publications

References 60 publications

Heterogeneity and targeted therapy-induced adaptations in lung cancer revealed by longitudinal single-cell RNA sequencing

Heterogeneity and targeted therapy-induced adaptations in lung cancer revealed by longitudinal single-cell RNA sequencing

Bystander CD4+T cells infiltrate human tumors and are phenotypically distinct

Cancer Cell‐targeted and Activatable Photoimmunotherapy Spares T Cells in a 3D Coculture Model

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Bystander CD4⁺T cells infiltrate human tumors and are phenotypically distinct