Improved cancer immunotherapy by a CD25-mimobody conferring selectivity to human interleukin-2

Arenas-Ramirez, Natalia; Zou, Chao; Popp, Simone; Zingg, Daniel; Brannetti, Barbara; Wirth, Emmanuelle; Calzascia, Thomas; Kovařík, Jiří; Sommer, Lukas; Zenke, Gerhard; Woytschak, Janine; Regnier, Catherine H.; Katopodis, Andreas; Boyman, Onur

doi:10.1126/scitranslmed.aag3187

Cited by 117 publications

(154 citation statements)

References 37 publications

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“…Indeed, surface plasmon resonance and P-STAT5 data using immune effector cells and Tregs from PBMC are supportive of a complete absence of CD25 affinity. CEA-IL2v exhibits a similar mechanism as described for the IL-2-S4B6 complex 11,53 and the human CD25-mimobody described recently, 54 including the lack of preferential activation of Tregs, reduced potency in triggering Fas-mediated apoptosis (AICD), superior tolerability compared with a wild-type IL-2-based immunocytokine and reduced clearance resulting in superior PK due to the lack of binding to the peripheral and endothelial CD25 sink 11 …”

Section: Discussionmentioning

confidence: 67%

Cergutuzumab amunaleukin (CEA-IL2v), a CEA-targeted IL-2 variant-based immunocytokine for combination cancer immunotherapy: Overcoming limitations of aldesleukin and conventional IL-2-based immunocytokines

et al. 2017

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We developed cergutuzumab amunaleukin (CEA-IL2v, RG7813), a novel monomeric CEA-targeted immunocytokine, that comprises a single IL-2 variant (IL2v) moiety with abolished CD25 binding, fused to the C-terminus of a high affinity, bivalent carcinoembryonic antigen (CEA)-specific antibody devoid of Fc-mediated effector functions. Its molecular design aims to (i) avoid preferential activation of regulatory T-cells vs. immune effector cells by removing CD25 binding; (ii) increase the therapeutic index of IL-2 therapy by (a) preferential retention at the tumor by having a lower dissociation rate from CEA-expressing cancer cells vs. IL-2R-expressing cells, (b) avoiding any FcγR-binding and Fc effector functions and (c) reduced binding to endothelial cells expressing CD25; and (iii) improve the pharmacokinetics, and thus convenience of administration, of IL-2. The crystal structure of the IL2v-IL-2Rβγ complex was determined and CEA-IL2v activity was assessed using human immune effector cells. Tumor targeting was investigated in tumor-bearing mice using 89Zr-labeled CEA-IL2v. Efficacy studies were performed in (a) syngeneic mouse models as monotherapy and combined with anti-PD-L1, and in (b) xenograft mouse models in combination with ADCC-mediating antibodies. CEA-IL2v binds to CEA with pM avidity but not to CD25, and consequently did not preferentially activate Tregs. In vivo, CEA-IL2v demonstrated superior pharmacokinetics and tumor targeting compared with a wild-type IL-2-based CEA immunocytokine (CEA-IL2wt). CEA-IL2v strongly expanded NK and CD8+ T cells, skewing the CD8+:CD4+ ratio toward CD8+ T cells both in the periphery and in the tumor, and mediated single agent efficacy in syngeneic MC38-CEA and PancO2-CEA models. Combination with trastuzumab, cetuximab and imgatuzumab, all of human IgG1 isotype, resulted in superior efficacy compared with the monotherapies alone. Combined with anti-PD-L1, CEA-IL2v mediated superior efficacy over the respective monotherapies, and over the combination with an untargeted control immunocytokine. These preclinical data support the ongoing clinical investigation of the cergutuzumab amunaleukin immunocytokine with abolished CD25 binding for the treatment of CEA-positive solid tumors in combination with PD-L1 checkpoint blockade and ADCC competent antibodies.

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Section: Discussionmentioning

confidence: 67%

Cergutuzumab amunaleukin (CEA-IL2v), a CEA-targeted IL-2 variant-based immunocytokine for combination cancer immunotherapy: Overcoming limitations of aldesleukin and conventional IL-2-based immunocytokines

et al. 2017

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“…Similarly, blocking IL‐2 signalling may reprogramme Tregs, but IL‐2 signalling also stimulates natural killer cells and T‐cells; thus, its blockade may hinder the anti‐tumour activities of these cells. Efforts to direct these drugs exclusively to Tregs, such as with optimized antibodies that specifically deplete TI‐Tregs or engineered IL‐2 molecules that do not bind Tregs, may be critical to the success of targeting the IL‐2 pathway . Further work identifying target pathways that act selectively in TI‐Tregs combined with new strategies for selectively delivering drugs to TI‐Tregs will be needed to expand the repertoire of therapeutic options to reprogramme TI‐Tregs.…”

Section: Conclusion: Key Challenges and Next Stepsmentioning

confidence: 99%

Treg programming and therapeutic reprogramming in cancer

Ayala

DuPage

2019

Immunology

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Summary Overcoming the immunosuppressive tumour microenvironment is the major challenge impeding cancer immunotherapy today. Regulatory T‐cells (Tregs) are prevalent in nearly all cancers and, as immunosuppressive regulators of immune responses, they are the principal opponents of cancer immunotherapy. However, disabling Tregs systemically causes severe autoimmune toxicity, hastening the need for more selective methods to target intratumoural Tregs. In this review, we discuss a burgeoning new modality to specifically target tumour‐infiltrating Tregs (TI‐Tregs) by reprogramming their functionality from immunosuppressive to immune stimulatory within tumours. As the basis for therapeutic selectivity of TI‐Tregs, we will focus on the defining features of Tregs within cancer: their highly activated state controlled by the engagement of key surface receptors, their distinct metabolic programme, and their unique transcriptional programme. By identifying proteins and pathways that distinguish TI‐Tregs from other Tregs in the body, as well as from the beneficial antitumour effector T‐cells within tumours, we highlight mechanisms to selectively reprogramme TI‐Tregs for the treatment of cancer.

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“…22-24 These have been widely characterized 25,26 and have garnered recent clinical interest with the development of humanized equivalents. 27 …”

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confidence: 99%

Injectable Polymeric Cytokine-Binding Nanowires Are Effective Tissue-Specific Immunomodulators

et al. 2017

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Injectable nanomaterials that interact with the host immune system without surgical intervention present spatially anchored complements to cell transplantation and could offer improved pharmacokinetics compared to systemic cytokine therapy. Here we demonstrate fabrication of high aspect ratio polycaprolactone nanowires coupled with cytokine-binding antibodies that assemble into porous matrices when injected into the subcutaneous space. These structures are fabricated using a nanotemplating technique that allows for tunability of particle dimensions and utilize a straightforward maleimide conjugation chemistry to allow site-specific coupling to proteins. Nanowires are well tolerated in vivo and incite minimal inflammatory infiltrate. Nanowires conjugated with antibodies were designed to capture and potentiate endogenous interleukin-2 (IL-2), an important leukocyte activating cytokine. Together these nanowire-antibody matrices were capable of localizing endogenous IL-2 in the skin and activated targeted specific natural killer and T cell subsets, demonstrating both tissue- and cell-specific immune activation. These self-assembling nanowire matrices show promise as scaffolds to present engineered, local receptor–ligand interactions for cytokine-mediated disease.

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Improved cancer immunotherapy by a CD25-mimobody conferring selectivity to human interleukin-2

Cited by 117 publications

References 37 publications

Cergutuzumab amunaleukin (CEA-IL2v), a CEA-targeted IL-2 variant-based immunocytokine for combination cancer immunotherapy: Overcoming limitations of aldesleukin and conventional IL-2-based immunocytokines

Cergutuzumab amunaleukin (CEA-IL2v), a CEA-targeted IL-2 variant-based immunocytokine for combination cancer immunotherapy: Overcoming limitations of aldesleukin and conventional IL-2-based immunocytokines

Treg programming and therapeutic reprogramming in cancer

Injectable Polymeric Cytokine-Binding Nanowires Are Effective Tissue-Specific Immunomodulators

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