Low Expression of IL-15 and NKT in Tumor Microenvironment Predicts Poor Outcome of MYCN-Non-Amplified Neuroblastoma

Liao, Yu‐Mei; Hung, Tsai-Hsien; Tung, John K; Yu, John; Hsu, Ya‐Ling; Hung, Jung‐Tung; Yu, Alice L.

doi:10.3390/jpm11020122

Cited by 11 publications

(7 citation statements)

References 51 publications

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“…MYCN knockdown in high-expressing cell lines (SK-N-BE(2) and LAN-1) increased CCL2 mRNA transcript expression levels ( 50 ). Lower IL-15 and NKT cell immunoscores were found in MYCN -non-amplified samples in multiple databases of transcript expression in NBL, and IL-15 expression confirmed by RT-PCR in a separate sample of clinical cDNA NBL specimens ( 51 ). MYCN -amplified samples express high levels of the H3K9 histone-lysine methytransferases EHMT and EZH2, which directly contribute to low expression of CXCL9 and CXCL10 and a non-T cell-inflamed phenotype in primary tumor transcriptomic data as well as in human NBL cells, and can be reversed by targeted EHMT and EZH2 inhibitors ( 52 ).…”

Section: Immune Phenotypes Of Pediatric Solid Tumorsmentioning

confidence: 93%

Targeted immune activation in pediatric solid tumors: opportunities to complement local control approaches

2023

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Surgery or radiation therapy is nearly universally applied for pediatric solid tumors. In many cases, in diverse tumor types, distant metastatic disease is present and evades surgery or radiation. The systemic host response to these local control modalities may lead to a suppression of antitumor immunity, with potential negative impact on the clinical outcomes for patients in this scenario. Emerging evidence suggests that the perioperative immune responses to surgery or radiation can be modulated therapeutically to preserve anti-tumor immunity, with the added benefit of preventing these local control approaches from serving as pro-tumorigenic stimuli. To realize the potential benefit of therapeutic modulation of the systemic response to surgery or radiation on distant disease that evades these modalities, a detailed knowledge of the tumor-specific immunology as well as the immune responses to surgery and radiation is imperative. In this Review we highlight the current understanding of the tumor immune microenvironment for the most common peripheral pediatric solid tumors, the immune responses to surgery and radiation, and current evidence that supports the potential use of immune activating agents in the perioperative window. Finally, we define existing knowledge gaps that limit the current translational potential of modulating perioperative immunity to achieve effective anti-tumor outcomes.

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Section: Immune Phenotypes Of Pediatric Solid Tumorsmentioning

confidence: 93%

Targeted immune activation in pediatric solid tumors: opportunities to complement local control approaches

2023

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“…iNKT cells have also been coengineered with GD2-CAR + IL-15. IL-15 is (1) a key cytokine for iNKT cell development and homoeostasis [181] , [182] , (2) protective towards iNKT cell inhibition mediated by TAM [183], and (3) low IL-15 or iNKT cell presence within the neuroblastoma TME is associated with poor patient outcome [184] . CD28 GD2/IL15 CAR iNKT cells displayed enhanced persistence, antitumour activity, and tumour localisation in neuroblastoma mouse xenografts, as well as a reduced exhaustion profile in vitro [185] .…”

Section: Inkt Cellsmentioning

confidence: 99%

Adoptive cell therapy in paediatric extracranial solid tumours: current approaches and future challenges

Zappa,

Vitali,

Anders

et al. 2023

European Journal of Cancer

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“…Moreover, two-thirds of human NB cell lines secrete CCL2, which mediates transendothelial migration of iNKTs in vitro, therefore, iNKT cells migrate toward NB cells in a CCL2-dependent manner, preferentially infiltrating MYCN nonamplified tumors that express CCL2 [49]. A study has recently shown that NKT cells can serve as a prognostic factor in MYCN-non-amplified NB [50]. Additionally, NB cells selectively express high levels of the ganglioside, GD2.…”

Section: Brain Cancers and Neuroblastomamentioning

confidence: 99%

Targeting Natural Killer T Cells in Solid Malignancies

Ingram

Madan

Merchant

et al. 2021

Cells

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Natural killer T (NKT) cells are a unique subset of lymphocytes that recognize lipid antigens in the context of the non-classical class I MHC molecule, CD1d, and serve as a link between the innate and adaptive immune system through their expeditious release of cytokines. Whereas NKT have well-established roles in mitigating a number of human diseases, herein, we focus on their role in cancer. NKT cells have been shown to directly and indirectly mediate anti-tumor immunity and manipulating their effector functions can have therapeutic significances in treatment of cancer. In this review, we highlight several therapeutic strategies that have been used to harness the effector functions of NKT cells to target different types of solid tumors. We also discuss several barriers to the successful utilization of NKT cells and summarize effective strategies being developed to harness the unique strengths of this potent population of T cells. Collectively, studies investigating the therapeutic potential of NKT cells serve not only to advance our understanding of this powerful immune cell subset, but also pave the way for future treatments focused on the modulation of NKT cell responses to enhance cancer immunotherapy.

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Low Expression of IL-15 and NKT in Tumor Microenvironment Predicts Poor Outcome of MYCN-Non-Amplified Neuroblastoma

Cited by 11 publications

References 51 publications

Targeted immune activation in pediatric solid tumors: opportunities to complement local control approaches

Targeted immune activation in pediatric solid tumors: opportunities to complement local control approaches

Adoptive cell therapy in paediatric extracranial solid tumours: current approaches and future challenges

Targeting Natural Killer T Cells in Solid Malignancies

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