Characterizing the Dysfunctional NK Cell: Assessing the Clinical Relevance of Exhaustion, Anergy, and Senescence

Judge, Sean J; Murphy, William J.; Canter, Robert J.

doi:10.3389/fcimb.2020.00049

Cited by 132 publications

(133 citation statements)

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“…Due to the uncoupling of clinical e cacy and CCR4 expression in eTreg cells and central-memory CD8 + T cells, we further explored the potential involvement of NK cell function in the clinical e cacy of mogamulizumab because mogamulizumab possesses enhanced antibody-dependent cellular cytotoxicity (ADCC) activity via a defucosylated Fc region 28 . NK cells exhibited an exhausted phenotype, which was determined by the expression of PD-1 and LAG-3, in some patients particularly in long-term survivors ( Figure 4A and 4B), indicating the presence of impaired ADCC activity in long-term survivors 29 . Patients, from whom the data regarding both CCR4 expression and NK cell exhaustion were available, were divided into long-term survivors and short-term survivors, and CCR4 expression and NK cell exhaustion were compared.…”

Section: Resultsmentioning

confidence: 99%

Unexpected central-memory CD8+ T cell reduction hampers the antitumor efficacy of mogamulizumab (anti-CC chemokine receptor 4 mAb) treatment

Maeda¹,

Wada²,

Saito³

et al. 2020

Preprint

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Developing Treg cell-targeted therapies is an important aspect in cancer immunotherapy. Here, we investigate anti-CCR4 mAb (mogamulizumab) with solid cancer patients in phase 1b clinical trial based on the predominant detection of CCR4-expressing eTreg cells in tumors. While eTreg cells in peripheral blood were significantly decreased after mogamulizumab administration in all patients, clinical responses were hardly detected. Comprehensive immune-monitoring revealed that concomitant reduction of central-memory CD8+ T cells with CCR4 expression, that reportedly play an important role in antitumor activity. This reduction was subsided in long survivors in whom central-memory CD8+ T cells possessed lower CCR4 expression and/or NK cells exhibited an exhausted phenotype. Thus, excess doses of mogamulizumab harboring enhanced antibody-dependent cellular cytotoxicity could unexpectedly deplete central-memory CD8+ T cells with CCR4 expression. We therefore need to carefully determine the optimal dose of mogamulizumab for successful clinical application as cancer immunotherapy to avoid unexpected depletion of effector components.

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Section: Resultsmentioning

confidence: 99%

Unexpected central-memory CD8+ T cell reduction hampers the antitumor efficacy of mogamulizumab (anti-CC chemokine receptor 4 mAb) treatment

Maeda¹,

Wada²,

Saito³

et al. 2020

Preprint

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“…NK cells have been found to be compromised in several cancers [3,6,[9][10][11][12][13]15,18,19,24,25,38]. NK cell contribution to tumour progression goes beyond the mechanism of tumour escape and immunosuppression [3,[10][11][12]24,25] .…”

Section: Discussionmentioning

confidence: 99%

“…As for several immune cells [3][4][5][6]8], NK cells have been described to acquire a tolerogenic behaviour and to be altered in their cytotoxic activities [3][4][5][6][10][11][12][13][14][15][16], they represent still an under investigated cell population and only few studies demonstrated pro-inflammatory angiogenic cancer cell growth promoting activities in cancers [3,[10][11][12]14]. Major mechanisms associated with impaired NK cell function in cancer patients, are downregulation of lytic perforin/granzyme production accompanied with reduction of degranulation capabilities, together with reduction of NKG2D (the major NK cell activation receptor) expression [17][18][19]. In prostate cancer, the ligands for NKp30 and NKp46 are expressed on NK cells from patients with primary tumours but not on benign prostate hyperplasia [20].…”

Section: Introductionmentioning

confidence: 99%

Prostate cancer peripheral blood NK cells show enhanced CD9, CD49a, CXCR4, CXCL8, MMP-9 production, and secrete monocyte-recruiting and polarizing factors

Baci

Gallazzi

Mortara

et al. 2020

Preprint

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ABSTRACTBackgroundNatural killer (NK) cells are effector lymphocytes of the innate immunity. Two major NK cell subsets are mostly present in the peripheral blood (pNKs): the cytotoxic CD56dimCD16+ NK cell subset (90-95% of pNKs), and the low cytotoxic, highly cytokine-producing CD56brightCD16-/low NK cell subset (5-10% of pNKs). It has been demonstrated that NK cells in peripheral blood of patients with several tumors are altered. We have shown that in NSCLC and colon cancer, tumor associated circulating NK (pTA-NK) and tumor infiltrating NK (TI-NK) are skewed towards the CD56brightCD16-/low phenotype. We have detected the production of pro-inflammatory and pro-angiogenic cytokines and chemokines. Other groups are reporting similar observations. There is still a lack of knowledge concerning the phenotype of pNK cells in prostate cancer (PCa). Here, we phenotypically and functionally characterized peripheral blood NK (pNK) from PCa patients (PCa pTA-NKs) and investigated their production of soluble factors, with endothelial cells and macrophage stimulatory action.MethodsNK cell subset distribution was investigated in the peripheral blood of PCa patients, by multicolor flow cytometry (FC) for surface antigens expression. Protein arrays were performed to characterize the secretome on FACS-sorted pNK cells. Secreted products from FACS-sorted PCa TA-NKs were used to characterize their production of pro-inflammatory molecules. Secreted products from FACS-sorted PCa pTA-NKs were also used to stimulate endothelial cells and monocytes and macrophages, determining their ability to recruit and polarize them. Alterations of endothelial cells and monocytes, following exposure to secreted products from FACS-sorted PCa pTA-NKs, was assessed by RT-PCR. To confirm these observations, secreted products from 3 different PCa (PC-3, DU-145, LNCaP) cell lines were used to assess their effects on human NK cell polarization, by multicolor flow cytometry.ResultsCirculating NK cells from prostate cancer patients have been studied before, mostly for their impaired lytic functions. However, here we are the first to report that circulating pNK cells from PCa patients acquire a CD56brightCD9+CD49a+CXCR4+ phenotype with pro-inflammatory properties. We observed a similar polarization of heathy-donor derived pNK cells exposed to secreted products of three different PCa cell lines. Increased production of CXCL8, CXCR4, MMP-9, pro-inflammatory and reduced production of TNFα, IFNγ and Granzyme-B was detected. PCa TA-NKs released factors able to support angiogenesis in vitro and increased the expression of CXCL8, ICAM-1 and VCAM-1 mRNA in endothelial cells, confirming a pro-inflammatory signature. Secretome analysis revealed the ability of PCa pTA-NKs to release pro-angiogenic cytokines/chemokines involved in monocyte recruitment and M2-like polarization. In experimental setting, secreted products from PCa pTA-NKs can recruit THP-1 monocyte and polarize THP-1-differentiated macrophage towards CD206/Arginase1/IL-10/CXCL8-expressing M2-like/TAMs.ConclusionsOur results show that PCa pTA-NKs are effector cells able to produce pro-inflammatory angiogenesis factors able to stimulate endothelial cells, attract monocytes and polarize macrophage to an M2-like type. Our data provides a rationale for the possible use of pNK profiling in clinical studies on PCaGRAPHICAL ABSTRACTGraphical Abstract:Representative cartoon illustrating the pro-angiogenic features of PCa pTA-NKs.A) direct effects of PCa pTA-NKs in supporting angiogenesis by interacting with endothelial cells. B) Proposed model for PCa pTA-NK pro-angiogenic activities via macrophage recruitment and polarization.

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“…Although many efforts have been expended to date to apply NK cells derived from peripheral blood to adoptive therapy of solid and hematopoietic cancers (Klingemann, 2015;Lim et al, 2015); this approach has encountered several pitfalls such as insu cient cell number, limited source accessibility, lower response to stimulants, decreased expansion potential and increased dysfunctionality. To address these limitations, other Moreover, surface receptors inducing inhibitory signals in NK cells, such as NKG2A are overexpressed in malignancies and chronic infections (Chester, Fritsch, & Kohrt, 2015;Judge et al, 2020). NKG2A is one of the most important inhibitory receptors which plays a role in the dysfunctionality of NK cells in the patients with the mentioned diseases through inducing IL-10 production.…”

Section: Introductionmentioning

confidence: 99%

“…NKG2A is one of the most important inhibitory receptors which plays a role in the dysfunctionality of NK cells in the patients with the mentioned diseases through inducing IL-10 production. Other inhibitory receptors having a prominent role in NK cells inactivation are Tim3 and PD-1 (Chan, Smyth, & Martinet, 2014;Judge et al, 2020;Vivier, Nunes, & Vely, 2004;Watzl & Long, 2010).…”

Section: Introductionmentioning

confidence: 99%

Overcoming the UCB HSCs –Derived NK Cells Dysfunctionality through Harnessing RAS/MAPK, IGF-1R and TGF-β Signaling Pathways

Shokouhifar

Sarab

Yazdanifar

et al. 2020

Preprint

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BackgroundNatural killer (NK) cells differentiated from umbilical cord blood (UCB) hematopoietic stem cells (HSCs) may be more suitable for cell-based immunotherapy compared to NK cells from adult donors. This is due to opportunity to choose alloreactive donors and potentially more robust in vivo expansion. However, the cytotoxicity of UCB-HSC derived NK cells against cancer cells might be suboptimal. To overcome this obstacle, we attempted to generate NK cells with potent antitumor activity by targeting RAS/MAPK, IGF-1R and TGF-β signaling pathways.MethodsThe CD34+ cells isolated from human UCB mononuclear cells through MACS with purity of (≥90%) were used to be differentiated into NK cells. After 21 days of induction with SFTG36, IS721 and IL-15/Hsp70 media, NK cells phenotype was studied and their cytotoxicity against K562 human erythroleukemia cell and SKOV3 ovarian carcinoma cells was analyzed.ResultsThe induced NK cells treated with SFTG36/I721 and SFTG36/IS721 growth factor cocktail expressed a phenotype with CD56+16+CD3- and NKG2D+ with mean fluorescence intensity (MFI) of 92.7%±1.45-168.00±19.20 and 93.23%±0.75-168.66±20.00 respectively. These NK cells once activated by IL-15, demonstrated a higher cytotoxicity against K562 (≥90%) (P ≤ 0.001) and SKOV3 tumor cells (≥65%) (P ≤ 0.001) compared to IL-15/Hsp70 activated NK cells.Conclusion The differentiation of ex vivo-expanded CD34+ cells through manipulation of RAS/MAPK, IGF-1R and TGF-β signaling pathways is an efficient approach for generating functional NK cells that can be used for cancer immunotherapy.

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Characterizing the Dysfunctional NK Cell: Assessing the Clinical Relevance of Exhaustion, Anergy, and Senescence

Cited by 132 publications

References 158 publications

Unexpected central-memory CD8+ T cell reduction hampers the antitumor efficacy of mogamulizumab (anti-CC chemokine receptor 4 mAb) treatment

Unexpected central-memory CD8+ T cell reduction hampers the antitumor efficacy of mogamulizumab (anti-CC chemokine receptor 4 mAb) treatment

Prostate cancer peripheral blood NK cells show enhanced CD9, CD49a, CXCR4, CXCL8, MMP-9 production, and secrete monocyte-recruiting and polarizing factors

Overcoming the UCB HSCs –Derived NK Cells Dysfunctionality through Harnessing RAS/MAPK, IGF-1R and TGF-β Signaling Pathways

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