GSK3 Inhibition Drives Maturation of NK Cells and Enhances Their Antitumor Activity

Cichocki, Frank; Valamehr, Bahram; Bjordahl, Ryan; Zhang, Bin; Rezner, Betsy; Rogers, Paul; Gaidarova, Svetlana; Moreno, Sandra; Tuininga, Katie; Dougherty, Phillip M.; McCullar, Valarie; Howard, Peter K.; Sarhan, Dhifaf; Taras, Emily; Schlums, Heinrich; Abbot, Stewart; Shoemaker, Daniel; Bryceson, Yenan T.; Blazar, Bruce R.; Wolchko, Scott; Cooley, Sarah; Miller, Jeffrey S.

doi:10.1158/0008-5472.can-17-0799

Cited by 116 publications

(100 citation statements)

References 31 publications

(34 reference statements)

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“…The GSK3 kinase may also control T-bet expression in NK cells. Indeed, pharmacological inhibition of GS3K induces an increase in T-bet, Zeb2, and Blimp1 expression in NK cells and greatly enhances their effector functions and anti-tumor potential [132]. A similar effect was observed in CD8 T cells upon combined blockade of CTLA-4, PD-1, and Lag-3 [133].…”

Section: Other Pathwaysmentioning

confidence: 84%

T‐bet and Eomes govern differentiation and function of mouse and human NK cells and ILC1

et al. 2018

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T-bet and Eomes are T-box transcription factors that drive the differentiation and function of cytotoxic lymphocytes such as NK cells. Their DNA-binding domains are highly similar, suggesting redundant transcriptional activity. However, while these transcription factors have different patterns of expression, the phenotype of loss-of-function mouse models suggests that they play distinct roles in the development of NK cells and other innate lymphoid cells (ILCs). Recent technological advances using reporter mice and conditional knockouts were fundamental in defining the regulation and function of these factors at steady state and during pathological conditions such as various types of cancer or infection. Here, we review these recent developments, focusing on NK cells as prototypical cytotoxic lymphocytes and their development, and also discuss parallels between NK cells and T cells. We also examine the role of T-bet and Eomes in human NK cells and ILC1s. Considering divergent findings on mouse and human ILC1s, we propose that NK cells are defined by coexpression of T-bet and Eomes, while ILC1s express only one of these factors, either T-bet or Eomes, depending on the tissue or the species.

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Section: Other Pathwaysmentioning

confidence: 84%

T‐bet and Eomes govern differentiation and function of mouse and human NK cells and ILC1

et al. 2018

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“…More attention should be devoted to developing products with defined functional characteristics. Focusing on the functional attributes of adaptive NK cells, Cichocki et al (2017) discovered that adding a small-molecule inhibitor of glycogen synthase kinase 3 to peripheral blood NK cells from a CMV-seropositive donor expanded ex vivo with IL-15 for one week resulted in an enriched population of adaptive CD57 + NKG2C ++ NK cells. This outcome was linked to the expression of several transcription factors associated with late-stage NK cell maturation, including T-BET, ZEB2, and BLIMP-1, without affecting cell viability or proliferation.…”

Section: Nk Cell Expansion Strategies Allow the Development Of Diversmentioning

confidence: 99%

Natural Killer Cells in Cancer Immunotherapy

Miller

Lanier

2019

Annu. Rev. Cancer Biol.

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119

111

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Natural killer (NK) cells have evolved to complement T and B cells in host defense against pathogens and cancer. They recognize infected cells and tumors using a sophisticated array of activating, costimulatory, and inhibitory receptors that are expressed on NK cell subsets to create extensive functional diversity. NK cells can be targeted to kill with exquisite antigen specificity by antibody-dependent cellular cytotoxicity. NK and T cells share many of the costimulatory and inhibitory receptors that are currently under evaluation in the clinic for cancer immunotherapy. As with T cells, genetic engineering is being employed to modify NK cells to specifically target them to tumors and to enhance their effector functions. As the selective pressures exerted by immunotherapies to augment CD8+T cell responses may result in loss of MHC class I, NK cells may provide an important fail-safe to eliminate these tumors by their capacity to eliminate tumors that are “missing self.”

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“…These KIR + NKG2C + CD57 + highly cytotoxic and mature NK cells are selectively expanded from CMV+ donor NK cell. Mature, adaptive NK cells do not proliferate well, instead immature NK cells were maturated using a pharmacological inhibitor of GSK3β kinase (Cichocki et al, 2017). Otherwise, NKG2C + NK cells are selectively activated and expanded using human HLA-E expressing feeder cells (Liu et al, 2017).…”

Section: Discussionmentioning

confidence: 99%

The CD56bright CD62L+ NKG2A+ immature cell subset is dominantly expanded in human cytokine-induced memory-like NK cells

Jin

Ahn

Kim³

et al. 2018

Preprint

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Recent studies have revealed immunological memory of NK cells. Short-term in vitro cytokine stimulation also induces NK cell memory, but heterogeneous cell subsets within the cytokine-induced memory-like (CIML) NK cells has not been elucidated.Here we found that the dominant cell subset in human CIML NK cells are immature CD56 bright CD62L + cells, and they were selectively expanded CD56 bright CD16 − CD62L + NK cells. Although these cells acquired KIR expression after the cytokine stimulation, sustained NKG2A expression inhibits cytotoxicity against HLA-E + target cells. In contrast, another checkpoint molecule LAG-3 is induced mainly on KIR + NKG2C + minor CIML NK cells. Our findings imply targeting NKG2A and LAG-3 should be considered for CIML NK cell-based immunotherapy.

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GSK3 Inhibition Drives Maturation of NK Cells and Enhances Their Antitumor Activity

Cited by 116 publications

References 31 publications

T‐bet and Eomes govern differentiation and function of mouse and human NK cells and ILC1

T‐bet and Eomes govern differentiation and function of mouse and human NK cells and ILC1

Natural Killer Cells in Cancer Immunotherapy

The CD56bright CD62L+ NKG2A+ immature cell subset is dominantly expanded in human cytokine-induced memory-like NK cells

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