Prolonged IKKβ Inhibition Improves Ongoing CTL Antitumor Responses by Incapacitating Regulatory T Cells

Heuser, Claudia; Gotot, Janine; Piotrowski, Eveline Christina; Philipp, Marie‐Sophie; Courrèges, Christina Johanna Felicia; Otte, Martin Sylvester; Guo, Lei; Schmid-Burgk, Jonathan L.; Hornung, Veit; Heine, Annkristin; Knolle, Percy A.; Garbi, Natalio; Serfling, Edgar; Evaristo, César; Thaiss, Friedrich; Kurts, Christian

doi:10.1016/j.celrep.2017.09.082

Cited by 20 publications

(34 citation statements)

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“…In our experiments, deletion of NEMO inhibited canonical NF-kB pathway activation, whereas IKK-2 kinase deletion allowed canonical NF-kB activation, probably via NEMO-IKK-1 complexes or a further kinase so far not identified in our experiments. As shown in another of our publications, (21) mice lacking IKK-2 in mature T reg cells developed scurfylike immunopathology caused by the death of peripheral FoxP3 + T reg cells and pharmacological IKK-2 inhibition down-regulated FoxP3 and CD25 expression. In contrast, activated cytotoxic T lymphocytes were resistant to IKK-2 inhibition, because other pathways-in particular, nuclear factor of activated T cells-1 signaling.…”

Section: Discussionsupporting

confidence: 69%

“…A study published from our laboratory by Gotot et al (20) showed that systemic IKK-2 inhibition after the induction of the disease increased renal injury in the NTN model and that activated cytotoxic T lymphocytes were resistant to IKK-2 inhibition because of other pathways-in particular, nuclear factor of activated T-cell signaling (21). NF-kB activation was demonstrated by our group after ischemia-reperfusion kidney injury, and more Th17 cells were found in ischemic CD4xNEMO D mice but not in CD4xIKK2 D mice (22).…”

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confidence: 99%

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T‐lymphocyte–specific knockout of IKK‐2 or NEMO induces T _h 17 cells in an experimental nephrotoxic nephritis mouse model

et al. 2018

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Experimental nephrotoxic serum nephritis (NTN) is a model for T‐cell–mediated human rapid progressive glomerulonephritis. T‐cell receptor stimulation involves intracellular signaling events that ultimately lead to the activation of transcription factors, such as NF‐κB. We explored the involvement of the NF‐κB components IKK‐2 and NEMO in NTN, by using cell‐specific knockouts of IKK‐2 and NEMO in CD4+ T lymphocytes. Our results demonstrate that although the course of disease was not grossly altered in CD4xIKK2Δ and CD4xNEMOΔ animals, renal regulatory T cells were significantly reduced and T helper (Th)1 and Th17 cells significantly increased in both knockout mouse groups. The expression of the renal cytokines and chemokines IL‐1β, CCL‐2, and CCL‐20 was also significantly altered in both knockout mice. Lymphocyte transcriptome analysis confirmed the increased expression of Th17‐related cytokines in spleen CD4+ T cells. Moreover, our array data demonstrate an interrupted canonical NF‐κB pathway and an increased expression of noncanonical NF‐κB pathway–related genes in nephritic CD4xNEMOΔ mice, highlighting different downstream effects of deletion of IKK‐2 or NEMO in T lymphocytes. We propose that better understanding of the role of IKK‐2 and NEMO in nephritis is essential for the clinical application of kinase inhibitors in patients with glomerulonephritis.—Guo, L., Huang, J., Chen, M., Piotrowski, E., Song, N., Zahner, G., Paust, H.‐J., Alawi, M., Geffers, R., Thaiss, F. T‐lymphocyte–specific knockout of IKK‐2 or NEMO induces Th17 cells in an experimental nephrotoxic nephritis mouse model. FASEB J. 33, 2359–2371 (2019). http://www.fasebj.org

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Section: Discussionsupporting

confidence: 69%

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confidence: 99%

T‐lymphocyte–specific knockout of IKK‐2 or NEMO induces T _h 17 cells in an experimental nephrotoxic nephritis mouse model

et al. 2018

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“…As described earlier, patients with rare homozygous deletion of the IKBKB gene typically lack Treg cells [ 141 ]. Consistent with this, prolonged IKKβ inhibition was recently shown to partially deplete circulating FOXP3+ Treg cells, due to their dependence on NF-κB signalling for survival [ 198 ]. Consequently, administration of an IKKβ inhibitor after tumour vaccination in a mouse melanoma model enhanced the CTL-dependent anti-tumour response and delayed tumour growth, identifying IKKβ as a potential druggable immune checkpoint.…”

Section: Recent Therapeutic Opportunities To Target Ikkβmentioning

confidence: 64%

“…For example, genetic deletion of IKKβ in T-cells abrogated the anti-tumour response in mice with fibrosarcoma [ 199 ]. Indeed, Heuser et al observed that high doses of IKKβ inhibitor suppressed CTL responses in their model [ 198 ]. This dosage effect was explained by the fact that Tregs were more sensitive than CTLs to IKKβ inhibition due to a greater reliance on NF-κB signalling for survival.…”

Section: Recent Therapeutic Opportunities To Target Ikkβmentioning

confidence: 99%

Targeting IKKβ in Cancer: Challenges and Opportunities for the Therapeutic Utilisation of IKKβ Inhibitors

Prescott

Cook

2018

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Deregulated NF-κB signalling is implicated in the pathogenesis of numerous human inflammatory disorders and malignancies. Consequently, the NF-κB pathway has attracted attention as an attractive therapeutic target for drug discovery. As the primary, druggable mediator of canonical NF-κB signalling the IKKβ protein kinase has been the historical focus of drug development pipelines. Thousands of compounds with activity against IKKβ have been characterised, with many demonstrating promising efficacy in pre-clinical models of cancer and inflammatory disease. However, severe on-target toxicities and other safety concerns associated with systemic IKKβ inhibition have thus far prevented the clinical approval of any IKKβ inhibitors. This review will discuss the potential reasons for the lack of clinical success of IKKβ inhibitors to date, the challenges associated with their therapeutic use, realistic opportunities for their future utilisation, and the alternative strategies to inhibit NF-κB signalling that may overcome some of the limitations associated with IKKβ inhibition.

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“…It is well known that once T cells (CD3+) are activated to differentiate into cytotoxic T lymphocytes (CTLs, CD8+), they would secret IFN‐γ, granzyme, and so on to activate cell apoptosis pathway such as activating caspase‐3 to kill the tumor cells. Therefore, we collected the distant tumors in all the treated mice on day 36 to measure the tumor‐infiltrating CD3+CD8+ T cells and investigated the caspase‐3 expression within those tumors . For the blank control administrated with PBS, the tumors displayed a weak intensity of CD3+, CD8+, and caspase‐3+ signals, indicating the poor immune induction (Figure I,J; and Figures S13 and S14, Supporting Information).…”

Section: Methodsmentioning

confidence: 99%

Expandable Immunotherapeutic Nanoplatforms Engineered from Cytomembranes of Hybrid Cells Derived from Cancer and Dendritic Cells

et al. 2019

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Using the cytomembranes (FMs) of hybrid cells acquired from the fusion of cancer and dendritic cells (DCs), this study offers a biologically derived platform for the combination of immunotherapy and traditional oncotherapy approaches. Due to the immunoactivation implicated in the cellular fusion, FMs can effectively express whole cancer antigens and immunological co‐stimulatory molecules for robust immunotherapy. FMs share the tumor's self‐targeting character with the parent cancer cells. In bilateral tumor‐bearing mouse models, the FM‐coated nanophotosensitizer causes durable immunoresponse to inhibit the rebound of primary tumors post‐nanophotosensitizer‐induced photodynamic therapy (PDT). The FM‐induced immunotherapy displays ultrahigh antitumor effects even comparable to that of PDT. On the other hand, PDT toward primary tumors enhances the immunotherapy‐caused regression of the irradiation‐free distant tumors. Consequently, both the primary and the distant tumors are almost completely eliminated. This tumor‐specific immunotherapy‐based nanoplatform is potentially expandable to multiple tumor types and readily equipped with diverse functions owing to the flexible nanoparticle options.

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Prolonged IKKβ Inhibition Improves Ongoing CTL Antitumor Responses by Incapacitating Regulatory T Cells

Cited by 20 publications

References 44 publications

T‐lymphocyte–specific knockout of IKK‐2 or NEMO induces T _h 17 cells in an experimental nephrotoxic nephritis mouse model

T‐lymphocyte–specific knockout of IKK‐2 or NEMO induces T _h 17 cells in an experimental nephrotoxic nephritis mouse model

Targeting IKKβ in Cancer: Challenges and Opportunities for the Therapeutic Utilisation of IKKβ Inhibitors

Expandable Immunotherapeutic Nanoplatforms Engineered from Cytomembranes of Hybrid Cells Derived from Cancer and Dendritic Cells

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Prolonged IKKβ Inhibition Improves Ongoing CTL Antitumor Responses by Incapacitating Regulatory T Cells

Cited by 20 publications

References 44 publications

T‐lymphocyte–specific knockout of IKK‐2 or NEMO induces T h 17 cells in an experimental nephrotoxic nephritis mouse model

T‐lymphocyte–specific knockout of IKK‐2 or NEMO induces T h 17 cells in an experimental nephrotoxic nephritis mouse model

Targeting IKKβ in Cancer: Challenges and Opportunities for the Therapeutic Utilisation of IKKβ Inhibitors

Expandable Immunotherapeutic Nanoplatforms Engineered from Cytomembranes of Hybrid Cells Derived from Cancer and Dendritic Cells

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T‐lymphocyte–specific knockout of IKK‐2 or NEMO induces T _h 17 cells in an experimental nephrotoxic nephritis mouse model

T‐lymphocyte–specific knockout of IKK‐2 or NEMO induces T _h 17 cells in an experimental nephrotoxic nephritis mouse model