The bispecific immunoligand ULBP2‐aCEA redirects natural killer cells to tumor cells and reveals potent anti‐tumor activity against colon carcinoma

Rothe, Achim; Jachimowicz, Ron D.; Borchmann, Sven; Madlener, Marie; Keßler, Jörg; Reiners, Katrin S.; Sauer, Maike; Hansen, Hinrich P.; Ullrich, Roland T.; Chatterjee, Sampurna; Borchmann, Peter; Yazaki, Paul J.; Koslowsky, Thomas C.; Engert, Andreas; Heukamp, Lukas C.; Hallek, Michael; Strandmann, Elke Pogge von

doi:10.1002/ijc.28609

Cited by 52 publications

(36 citation statements)

References 39 publications

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“…The first of this kind was a RAET1H-anti-CD138 fusion protein that bound to CD138, which is overexpressed in multiple myeloma 186 , and crosslinked NKG2D on NK cells. Similarly, a RAET1H-anti-carcinoembryonic antigen (CEA) bispecific protein showed significant in vitro and in vivo efficacy against colon carcinoma 187 . Another study used recombinant MICA conjugated to mono clonal antibodies specific for CEA, HER2 or CD20, and their use resulted in NKG2D-dependent tumour cell lysis by NK cells 188 .…”

Section: Using Nk Cells For Cancer Therapymentioning

confidence: 99%

NK cells and cancer: you can teach innate cells new tricks

2015

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Section: Using Nk Cells For Cancer Therapymentioning

confidence: 99%

NK cells and cancer: you can teach innate cells new tricks

2015

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“…19 We reported the first such immunoligand, ULBP2-BB4 (scFv against CD138), which successfully activated and retargeted NK cells through ULBP2 against CD138-positive multiple myeloma cells both in vitro and in vivo. 20 Subsequently, two additional immunoligands in similar formats, ULBP2-aCEA (scFv against CEA) 21 and ULBP2-aPSMA (scFv against PSMA) 22 and immunoligands fused to other ligands, [23][24][25] validated our approach. Several trispecific immunoconstructs targeting the FcgRIIIa receptor on NK cells have been developed and compared with their bispecific counterparts.…”

Section: Introductionmentioning

confidence: 81%

“…19,30 So far, these novel approaches mainly involved bispecific recombinant proteins by our group and others to exploit NKG2D-dependent NK cell activation against tumor. [19][20][21] In this study, our strategy was to design NKG2D-triggering triplebodies that involved targeting of CD19 antigen or CD19/CD33 in combination. ULBP2-aCD19-aCD19 targets CD19 on CLL cells by two subsequent antiCD19 scFvs separated by 20 amino acid long Gly/Ser linker.…”

Section: Discussionmentioning

confidence: 99%

“…We previously reported the activation of NKT and T cells from spleen and peripheral blood of a syngeneic mouse model by ULBP2-aCEA immunoligand. 21 Although, g/d T cells represent a small subset of T cells, NKG2D co-stimulation on Vg9Vd2 T cells promotes secretion of IFNg, TNFa and cytotoxicity. 39 Recently, recombinant antibodies could successfully retarget g/d T cell effector functions against HER2-positive tumor cells.…”

Section: Discussionmentioning

confidence: 99%

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Mono- and dual-targeting triplebodies activate natural killer cells and have anti-tumor activityin vitroandin vivoagainst chronic lymphocytic leukemia

et al. 2016

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Chronic lymphocytic leukemia (CLL) is the most common form of leukemia that affects B lymphocytes in adults. Natural killer (NK) cells in CLL patients are intrinsically potent but display poor in situ effector functions. NKG2D is an activating receptor found on NK and CD8 C T cells and plays a role in immunosurveillance of CLL. In this study, we developed mono-and dual-targeting triplebodies utilizing a natural ligand for human NKG2D receptor (ULBP2) to retarget NK cells against tumor cells. Triplebodies in both formats showed better ability to induce NK-cell-dependent killing of target cells compared to bispecific counterparts. A mono-targeting triplebody ULBP2-aCD19-aCD19 successfully triggered NK cell effector functions against CLL cell line MEC1 and primary tumor cells in allogenic and autologous settings. Additionally, a dual-targeting triplebody ULBP2-aCD19-aCD33 specific for two distinct tumor-associated antigens was developed to target antigen loss variants, such as mixed lineage leukemia (MLL). Of note, this triplebody exhibited cytotoxic activity against CD19/CD33 double positive cells and retained its binding features even in the absence of one of the tumor antigens. Further, ULBP2-aCD19-aCD19 showed significant in vivo activity in immune-deficient (NSG) mouse model transplanted with CLL cell line as target cells and human immune cells as an effector population providing a proof-of-principle for this therapeutic concept.

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“…Many researchers have already harness the potential of NK cells by developing immuno ligands that target NKG2D via its cognate ligand (ULBP2) and bind to the target cells via an antibody derived single chain, which is specific for a tumour-associated antigen [15,16]. These immuno ligands have demonstrated antitumour activity both in vitro and in vivo.…”

Section: Conceptual Papermentioning

confidence: 99%

Cancer Immunotherapy: New Technology to Target Cancer Cells

Potdar¹

2016

MOJCSR

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The bispecific immunoligand ULBP2‐aCEA redirects natural killer cells to tumor cells and reveals potent anti‐tumor activity against colon carcinoma

Cited by 52 publications

References 39 publications

NK cells and cancer: you can teach innate cells new tricks

NK cells and cancer: you can teach innate cells new tricks

Mono- and dual-targeting triplebodies activate natural killer cells and have anti-tumor activityin vitroandin vivoagainst chronic lymphocytic leukemia

Cancer Immunotherapy: New Technology to Target Cancer Cells

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