Receptor-gated IL-2 delivery by an anti-human IL-2 antibody activates regulatory T cells in three different species

Karakus, Ufuk; Şahin, Dilara; Mittl, Peer R. E.; Mooij, Petra; Koopman, Gerrit; Boyman, Onur

doi:10.1126/scitranslmed.abb9283

Cited by 62 publications

(64 citation statements)

References 59 publications

(106 reference statements)

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“…For quantification of the main T cell subsets, blood samples were processed in the accredited routine immunology laboratory at University Hospital Zurich. Flow cytometry staining, assessment and analysis was done as established, 58,59 using the reagents and methodology detailed in the Appendix S1.…”

Section: Flow Cytometrymentioning

confidence: 99%

Profound dysregulation of T cell homeostasis and function in patients with severe COVID‐19

Adamo

Chevrier

Cervia

et al. 2021

Allergy

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Section: Flow Cytometrymentioning

confidence: 99%

Profound dysregulation of T cell homeostasis and function in patients with severe COVID‐19

Adamo

Chevrier

Cervia

et al. 2021

Allergy

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“…The second group of antibodies is used to amplify the immune suppressive function of IL-2 by activating T reg cells. 18 JES6-1, 13 UFKA-20, 19 and 5344 18 (anti-hIL-2 antibody, BD biosciences) are good examples. JES6-1 antibody blocks IL-2Rβ binding site and left IL-2Rα binding site as accessible, therefore JES6-1 antibody complexed mouse IL-2 can bind to IL-2Rα on immunosuppressive T cells, and then JES6-1 antibody is released from IL-2 to allow IL-2 interaction with IL-2Rβ and IL-2Rγ for activation of IL-2 signaling.…”

Section: Discussionmentioning

confidence: 99%

Crystal structure of human interleukin-2 in complex with TCB2, a new antibody-drug candidate with antitumor activity

Kim

Lee²,

Park

et al. 2021

OncoImmunology

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Immunotherapy via interleukin-2 (IL-2) mediated activation of anti-tumor immune response is a promising approach for cancer treatment. The multi-potent cytokine, IL-2 has a central role in immune cell activation and homeostasis. Since IL-2 preferentially activates immunosuppressive T regulatory cells by IL-2Rα dependent manner, blocking IL-2:IL-2Rα interaction is a key to amplify the IL-2 activity in effector T cells toward anti-tumor response. Anti-IL-2 monoclonal antibodies are good candidates to control the IL-2:IL-2Rα interaction. In a previous study, we developed a new IL-2Rα mimetic antibody, TCB2, and showed that the human IL-2(hIL-2):TCB2 complex can stimulate T effector cells specifically and elicit potent anti-cancer immunotherapeutic effect, especially when administered in combination with immune checkpoint inhibitors. To understand the molecular mechanism, we determined the crystal structure of TCB2-Fab in a complex with hIL-2 at 2.5 Å resolution. Our structural analysis reveals that TCB2 binds to the central area of the hIL-2Rα binding region on hIL-2, and binding angle and epitope are different from previously known hIL-2Rα mimicking antibody NARA1 which recognizes the top part of hIL-2. TCB2 binding to hIL-2 also induces an allosteric effect that increases the affinity for the hetero-dimeric hIL-2 receptor, IL-2R(β + γ), on effector T cells.

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“…These include PEGylated IL-2 (NKTR-358 "LY3471851") (303), which induced clinical response and dose-dependent changes in Treg functional markers in a phase I trial in mild-to-moderate SLE, various IL-2:IL-2 Ab complexes described as CD25-directed IL-2cx (283,284) and CD25-IL2 fusion proteins (287,288). Anti-IL-2 antibodies that form complex with IL-2 can attenuate the IL2R signal by sterically inhibiting the IL-2: IL2R interactions but they can also modify the IL-2 structure to influence the bias with which it interacts with the receptor subunits (285,286). Likewise, CD25-IL-2 fusion proteins formed multimers via intermolecular binding, effectively limiting the amount of free IL-2 that could bind to CD25 on cell surfaces.…”

Section: Engineered Il-2 Therapymentioning

confidence: 99%

Emerging Therapeutics for Immune Tolerance: Tolerogenic Vaccines, T cell Therapy, and IL-2 Therapy

2021

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Autoimmune diseases affect roughly 5-10% of the total population, with women affected more than men. The standard treatment for autoimmune or autoinflammatory diseases had long been immunosuppressive agents until the advent of immunomodulatory biologic drugs, which aimed at blocking inflammatory mediators, including proinflammatory cytokines. At the frontier of these biologic drugs are TNF-α blockers. These therapies inhibit the proinflammatory action of TNF-α in common autoimmune diseases such as rheumatoid arthritis, psoriasis, ulcerative colitis, and Crohn’s disease. TNF-α blockade quickly became the “standard of care” for these autoimmune diseases due to their effectiveness in controlling disease and decreasing patient’s adverse risk profiles compared to broad-spectrum immunosuppressive agents. However, anti-TNF-α therapies have limitations, including known adverse safety risk, loss of therapeutic efficacy due to drug resistance, and lack of efficacy in numerous autoimmune diseases, including multiple sclerosis. The next wave of truly transformative therapeutics should aspire to provide a cure by selectively suppressing pathogenic autoantigen-specific immune responses while leaving the rest of the immune system intact to control infectious diseases and malignancies. In this review, we will focus on three main areas of active research in immune tolerance. First, tolerogenic vaccines aiming at robust, lasting autoantigen-specific immune tolerance. Second, T cell therapies using Tregs (either polyclonal, antigen-specific, or genetically engineered to express chimeric antigen receptors) to establish active dominant immune tolerance or T cells (engineered to express chimeric antigen receptors) to delete pathogenic immune cells. Third, IL-2 therapies aiming at expanding immunosuppressive regulatory T cells in vivo.

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Receptor-gated IL-2 delivery by an anti-human IL-2 antibody activates regulatory T cells in three different species

Cited by 62 publications

References 59 publications

Profound dysregulation of T cell homeostasis and function in patients with severe COVID‐19

Profound dysregulation of T cell homeostasis and function in patients with severe COVID‐19

Crystal structure of human interleukin-2 in complex with TCB2, a new antibody-drug candidate with antitumor activity

Emerging Therapeutics for Immune Tolerance: Tolerogenic Vaccines, T cell Therapy, and IL-2 Therapy

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