Emergence of NK Cell Hyporesponsiveness after Two IL-15 Stimulation Cycles

Frutoso, Marie; Morisseau, Sébastien; Tamzalit, Fella; Quéméner, Agnès; Meghnem, Dihia; Leray, Isabelle; Jacques, Yannick; Mortier, Erwan

doi:10.4049/jimmunol.1800086

Cited by 18 publications

(28 citation statements)

References 62 publications

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“…98 Moreover, two recent studies also show that repeated cycles of N-803 injection may lead to reduced biological responsiveness in NK cells of SIV + macaque 99 and, in a phase 1b trial, in patients with metastatic non-small cell lung cancer. 100 These data open up two questions: NK hyporesponsiveness observed in cancer patients receiving repeated cycles of IL-15 or soluble complex is induced by the contemporary expansion of an inhibitory T cell subset as reported in mice 84 or may be directly induced by IL-15 and/or the super-agonist complex? If the second hypothesis holds true, ex vivo protocols for the expansion of NK cells intended to be reinjected in patients with cancer as a complementary immunologic treatment should be Open access solves the above mentioned problems (unpublished results).…”

Section: Clinical Trials Rhil-15 Is Currently Under Investigation In mentioning

confidence: 97%

“…These data highlights as an excessive stimulation of NK cells by sIL-15 and sIL-15/IL-15Rα complexes may induce NK hyporesponsiveness. 84 Indeed, prolonged NK cell activation using ionomycin as well as repeated exposure to Toll-like receptors (TLRs) agonists and 85 repeated injections of interferon (IFN)-α 86 induced decreased cytolytic function and cytokine production. 87 Both TLRs and IFN-α stimulation increase production of IL-15, IL-15Rα and/or of the soluble complex 36 85 86 88 89 that are potentially responsible of NK cells exhaustion.…”

Section: Il-15 Sil-15/il-15rα Complex and Cancer Treatment Preclinicmentioning

confidence: 99%

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Interleukin-15 and cancer: some solved and many unsolved questions

Fiore

Matteo

Tumino

et al. 2020

J Immunother Cancer

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Soluble interleukin (IL)-15 exists under two forms: as monomer (sIL-15) or as heterodimeric complex in association with sIL-15Rα (sIL-15/IL-15Rα). Both forms have been successfully tested in experimental tumor murine models and are currently undergoing investigation in phase I/II clinical trials. Despite more than 20 years research on IL-15, some controversial issues remain to be addressed. A first point concerns the detection of the sIL-15/IL-15Rα in plasma of healthy donors or patients with cancer and its biological significance. The second and third unsolved question regards the protumorigenic role of the IL-15/IL-15Rα complex in human cancer and the detrimental immunological consequences associated to prolonged exposure of natural killer (NK) cells to both forms of soluble IL-15, respectively. Data suggest that in vivo prolonged or repeated exposure to monomeric sIL-15 or the soluble complex may lead to NK hypo-responsiveness through the expansion of the CD8+/CD44+ T cell subset that would suppress NK cell functions. In vitro experiments indicate that soluble complex and monomeric IL-15 may cause NK hyporesponsiveness through a direct effect caused by their prolonged stimulation, suggesting that this mechanism could also be effective in vivo. Therefore, a better knowledge of IL-15 and a more appropriate use of both its soluble forms, in terms of concentrations and time of exposure, are essential in order to improve their therapeutic use. In cancer, the overproduction of sIL-15/IL-15Rα could represent a novel mechanism of immune escape. The soluble complex may act as a decoy cytokine unable to efficiently foster NK cells, or could induce NK hyporesponsiveness through an excessive and prolonged stimulation depending on the type of IL-15Rα isoforms associated. All these unsolved questions are not merely limited to the knowledge of IL-15 pathophysiology, but are crucial also for the therapeutic use of this cytokine. Therefore, in this review, we will discuss key unanswered issues on the heterogeneity and biological significance of IL-15 isoforms, analyzing both their cancer-related biological functions and their therapeutic implications.

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Section: Clinical Trials Rhil-15 Is Currently Under Investigation In mentioning

confidence: 97%

Section: Il-15 Sil-15/il-15rα Complex and Cancer Treatment Preclinicmentioning

confidence: 99%

Interleukin-15 and cancer: some solved and many unsolved questions

Fiore

Matteo

Tumino

et al. 2020

J Immunother Cancer

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“…Since the 1980′s, impact of treatments with IFNα, IL-2, IL-12 or IL-15, on NK cells have been examined in mice. Unexpectedly, while a single treatment with one of the above-mentioned cytokines leads to an increased NK cell cytotoxic activity, multiple treatments with one cytokine was shown to be negatively correlated with NK cell cytotoxic activity [142,143,144,145,146,147,148]. This NK cell hyporesponsiveness driven by cytokines was shown to be systemic [144,148], indicating that the origin of this phenomenon was not linked to a redistribution to other organs.…”

Section: Nk Cell Hyporesponsiveness Emergence After Treatmentmentioning

confidence: 99%

“…However, similar to IL-15, repeated treatments with IL-15 agonists lead to NK cell hyporesponsiveness. This NK cell hyporesponsiveness following multiple treatments is systemic and characterized by impaired activation (altered balance of activating and inhibitory receptors, decreased expression of the CD69 early activation marker), reduced proliferation (decreased Ki67 expression, decreased Stat5 phosphorylation), and decreased anti-tumor activity (decreased clearance of B16F10 tumor cells in a metastatic model) [146,148]. Importantly, NK cell hyporesponsiveness following repeated treatment with IL-2, IL-15 or IL-15 agonists was not linked to a decreased expression of the CD122 CD132 chains [144,146,148] indicating that NK cells should be able to respond to the cytokines when re-injected (Figure 3).…”

Section: Nk Cell Hyporesponsiveness Emergence After Treatmentmentioning

confidence: 99%

“…In mice, one study hypothesized the implication of regulatory cells or immunosuppressive cytokines but lacked sufficient evidence [144]. Moreover, regulatory T cells, immunosuppressive cytokines such as IL-10 or TGFβ, and also IFNγ, were shown not to be involved in IL-15 repeated treatment [146,148]. Studies from Saito and colleagues in 1985 have shown that NK cell hyporesponsiveness following repeated treatment with cytokine was linked to a decreased percentage of large granular lymphocytes (LGL), the effector cell population responsible for NK cell-mediated cytotoxicity [142,143].…”

Section: Nk Cell Hyporesponsiveness Emergence After Treatmentmentioning

confidence: 99%

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NK Cell Hyporesponsiveness: More Is Not Always Better

Frutoso

Mortier

2019

IJMS

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Natural Killer (NK) cells are a type of cytotoxic lymphocytes that play an important role in the innate immune system. They are of particular interest for their role in elimination of intracellular pathogens, viral infection and tumor cells. As such, numerous strategies are being investigated in order to potentiate their functions. One of these techniques aims at promoting the function of their activating receptors. However, different observations have revealed that providing activation signals could actually be counterproductive and lead to NK cells’ hyporesponsiveness. This phenomenon can occur during the NK cell education process, under pathological conditions, but also after treatment with different agents, including cytokines, that are promising tools to boost NK cell function. In this review, we aim to highlight the different circumstances where NK cells become hyporesponsive and the methods that could be used to restore their functionality.

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2022 update on the scientific premise and clinical trials for IL-15 agonists as cancer immunotherapy

Peng

Zhao

2022

Journal of Leukocyte Biology

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Diverse cytokines and their receptors on immune cells constitute a highly complex network in the immune system. Some therapeutic cytokines and their derivatives have been approved for cancer treatment. IL‐15 is an immune‐regulating cytokine with multiple functions, among which the function of activating the immunity of cancer patients has great potential in cancer immunotherapy. In this review, we introduce the functions of IL‐15 and discuss its role in regulating the immune system in different immune cells. Meanwhile, we will address the applications of IL‐15 agonists in cancer immunotherapy and provide prospects for the next generation of therapeutic designs. Although many challenges remain, IL‐15 agonists offer a new therapeutic option in the future direction of cancer immunotherapy.

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Emergence of NK Cell Hyporesponsiveness after Two IL-15 Stimulation Cycles

Cited by 18 publications

References 62 publications

Interleukin-15 and cancer: some solved and many unsolved questions

Interleukin-15 and cancer: some solved and many unsolved questions

NK Cell Hyporesponsiveness: More Is Not Always Better

2022 update on the scientific premise and clinical trials for IL-15 agonists as cancer immunotherapy

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