Your search keyword '"Armin Ehninger"' showing total 46 results

1. Targeting senescent cells with NKG2D-CAR T cells

Author

Yushuang Deng, Avadh Kumar, Kan Xie, Kristina Schaaf, Enzo Scifo, Sarah Morsy, Tao Li, Armin Ehninger, Daniele Bano, and Dan Ehninger

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Cytology, QH573-671

Abstract

Abstract This study investigates the efficacy of NKG2D chimeric antigen receptor (CAR) engineered T cells in targeting and eliminating stress-induced senescent cells in vitro. Cellular senescence contributes to age-related tissue decline and is characterized by permanent cell cycle arrest and the senescence-associated secretory phenotype (SASP). Immunotherapy, particularly CAR-T cell therapy, emerges as a promising approach to selectively eliminate senescent cells. Our focus is on the NKG2D receptor, which binds to ligands (NKG2DLs) upregulated in senescent cells, offering a target for CAR-T cells. Using mouse embryonic fibroblasts (MEFs) and astrocytes (AST) as senescence models, we demonstrate the elevated expression of NKG2DLs in response to genotoxic and oxidative stress. NKG2D-CAR T cells displayed potent cytotoxicity against these senescent cells, with minimal effects on non-senescent cells, suggesting their potential as targeted senolytics. In conclusion, our research presents the first evidence of NKG2D-CAR T cells’ ability to target senescent brain cells, offering a novel approach to manage senescence-associated diseases. The findings pave the way for future investigations into the therapeutic applicability of NKG2D-targeting CAR-T cells in naturally aged organisms and models of aging-associated brain diseases in vivo.

Published

2024

2. Rapidly Switchable Universal CAR-T Cells for Treatment of CD123-Positive Leukemia

Author

Simon Loff, Josephine Dietrich, Jan-Erik Meyer, Julia Riewaldt, Johannes Spehr, Malte von Bonin, Cordula Gründer, Mridula Swayampakula, Kristin Franke, Anja Feldmann, Michael Bachmann, Gerhard Ehninger, Armin Ehninger, and Marc Cartellieri

Subjects

UniCAR, AML, ALL, CD123, CAR-T, immunotherapy, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Chimeric antigen receptor T cells (CAR-T) targeting CD19 or B cell maturation antigen (BCMA) are highly effective against B cell malignancies. However, application of CAR-T to less differentially expressed targets remains a challenge due to lack of tumor-specific antigens and CAR-T controllability. CD123, a highly promising leukemia target, is expressed not only by leukemic and leukemia-initiating cells, but also by myeloid, hematopoietic progenitor, and certain endothelial cells. Thus, CAR-T lacking fine-tuned control mechanisms pose a high toxicity risk. To extend the CAR-T target landscape and widen the therapeutic window, we adapted our rapidly switchable universal CAR-T platform (UniCAR) to target CD123. UniCAR-T efficiently eradicated CD123+ leukemia in vitro and in vivo. Activation, cytolytic response, and cytokine release were strictly dependent on the presence of the CD123-specific targeting module (TM123) with comparable efficacy to CD123-specific CAR-T in vitro. We further demonstrated a pre-clinical proof of concept for the safety-switch mechanism using a hematotoxicity mouse model wherein TM123-redirected UniCAR-T showed reversible toxicity toward hematopoietic cells compared to CD123 CAR-T. In conclusion, UniCAR-T maintain full anti-leukemic efficacy, while ensuring rapid controllability to improve safety and versatility of CD123-directed immunotherapy. The safety and efficacy of UniCAR-T in combination with TM123 will now be assessed in a phase I clinical trial (ClinicalTrials.gov: NCT04230265).

Published

2020

3. Evaluation of switch-mediated costimulation in trans on universal CAR-T cells (UniCAR) targeting CD123-positive AML

Author

Jan-Erik Meyer, Simon Loff, Josephine Dietrich, Johannes Spehr, Gabriel Jurado Jiménez, Malte von Bonin, Gerhard Ehninger, Marc Cartellieri, and Armin Ehninger

Subjects

chimeric antigen receptor (car), switchable car platform, costimulation in trans, 4-1bb, acute myeloid leukemia (aml), cd123, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Chimeric antigen receptor T cells (CAR-T) targeting CD19 have achieved significant success in patients with B cell malignancies. To date, implementation of CAR-T in other indications remains challenging due to the lack of truly tumor-specific antigens as well as control of CAR-T activity in patients. CD123 is highly expressed in acute myeloid leukemia (AML) blasts including leukemia-initiating cells making it an attractive immunotherapeutic target. However, CD123 expression in normal hematopoietic progenitor cells and endothelia bears the risk of severe toxicities and may limit CAR-T applications lacking fine-tuned control mechanisms. Therefore, we recently developed a rapidly switchable universal CAR-T platform (UniCAR), in which CAR-T activity depends on the presence of a soluble adapter called targeting module (TM), and confirmed clinical proof-of-concept for targeting CD123 in AML with improved safety. As costimulation via 4–1BB ligand (4–1BBL) can enhance CAR-T expansion, persistence, and effector functions, a novel CD123-specific TM variant (TM123-4-1BBL) comprising trimeric single-chain 4–1BBL was developed for transient costimulation of UniCAR-T cells (UniCAR-T) at the leukemic site in trans. TM123-4-1BBL-directed UniCAR-T efficiently eradicated CD123-positive AML cells in vitro and in a CDX in vivo model. Moreover, additional costimulation via TM123-4-1BBL enabled enhanced expansion and persistence with a modulated UniCAR-T phenotype. In addition, the increased hydrodynamic volume of TM123-4-1BBL prolonged terminal plasma half-life and ensured a high total drug exposure in vivo. In conclusion, expanding the soluble adapter optionality for CD123-directed UniCAR-T maintains the platforms high anti-leukemic efficacy and immediate control mechanism for a flexible, safe, and individualized CAR-T therapy of AML patients.

Published

2021

4. Characterization of a switchable chimeric antigen receptor platform in a pre-clinical solid tumor model

Author

Elham Pishali Bejestani, Marc Cartellieri, Ralf Bergmann, Armin Ehninger, Simon Loff, Michael Kramer, Johannes Spehr, Antje Dietrich, Anja Feldmann, Susann Albert, Martin Wermke, Michael Baumann, Mechthild Krause, Martin Bornhäuser, Gerhard Ehninger, Michael Bachmann, and Malte von Bonin

Subjects

chimeric antigen receptors, immune checkpoints, immunoevasion, prostate stem cell antigen, solid tumors, targeting module, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

The universal modular chimeric antigen receptor (UniCAR) platform redirects CAR-T cells using a separated, soluble targeting module with a short half-life. This segregation allows precise controllability and flexibility. Herein we show that the UniCAR platform can be used to efficiently target solid cancers in vitro and in vivo using a pre-clinical prostate cancer model which overexpresses prostate stem cell antigen (PSCA). Short-term administration of the targeting module to tumor bearing immunocompromised mice engrafted with human UniCAR-T cells significantly delayed tumor growth and prolonged survival of recipient mice both in a low and high tumor burden model. In addition, we analyzed phenotypic and functional changes of cancer cells and UniCAR-T cells in association with the administration of the targeting module to reveal potential immunoevasive mechanisms. Most notably, UniCAR-T cell activation induced upregulation of immune-inhibitory molecules such as programmed death ligands. In conclusion, this work illustrates that the UniCAR platform mediates potent anti-tumor activity in a relevant in vitro and in vivo solid tumor model.

Published

2017

5. A novel nanobody-based target module for retargeting of T lymphocytes to EGFR-expressing cancer cells via the modular UniCAR platform

Author

Susann Albert, Claudia Arndt, Anja Feldmann, Ralf Bergmann, Dominik Bachmann, Stefanie Koristka, Florian Ludwig, Pauline Ziller-Walter, Alexandra Kegler, Sebastian Gärtner, Marc Schmitz, Armin Ehninger, Marc Cartellieri, Gerhard Ehninger, Hans-Jürgen Pietzsch, Jens Pietzsch, Jörg Steinbach, and Michael Bachmann

Subjects

car, egfr, retargeting, t cell, t cell therapy, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Recent treatments of leukemias with chimeric antigen receptor (CAR) expressing T cells underline their impressive therapeutic potential. However, once adoptively transferred into patients, there is little scope left to shut them down after elimination of tumor cells or in case adverse side effects occur. This becomes of special relevance if they are directed against commonly expressed tumor associated antigens (TAAs) such as receptors of the ErbB family. To overcome this limitation, we recently established a modular CAR platform technology termed UniCAR. UniCARs are not directed against TAAs but instead against a unique peptide epitope on engineered recombinant targeting modules (TMs), which guide them to the target. In the absence of a TM UniCAR T cells are inactive. Thus an interruption of any UniCAR activity requires an elimination of unbound TM and the TM complexed with UniCAR T cells. Elimination of the latter one requires a disassembly of the UniCAR-TM complexes. Here, we describe a first nanobody (nb)-based TM directed against EGFR. The novel TM efficiently retargets UniCAR T cells to EGFR positive tumors and mediates highly efficient target-specific and target-dependent tumor cell lysis both in vitro and in vivo. After radiolabeling of the novel TM with 64Cu and 68Ga, we analyzed its biodistribution and clearance as well as the stability of the UniCAR-TM complexes. As expected unbound TM is rapidly eliminated while the elimination of the TM complexed with UniCAR T cells is delayed. Nonetheless, we show that UniCAR-TM complexes dissociate in vitro and in vivo in a concentration-dependent manner in line with the concept of a repeated stop and go retargeting of tumor cells via the UniCAR technology.

Published

2017

6. Characterization of a novel single-chain bispecific antibody for retargeting of T cells to tumor cells via the TCR co-receptor CD8.

Author

Irene Michalk, Anja Feldmann, Stefanie Koristka, Claudia Arndt, Marc Cartellieri, Armin Ehninger, Gerhard Ehninger, and Michael P Bachmann

Subjects

Medicine, Science

Abstract

There is currently growing interest in retargeting of effector T cells to tumor cells via bispecific antibodies (bsAbs). Usually, bsAbs are directed on the one hand to the CD3 complex of T cells and on the other hand to a molecule expressed on the surface of the target cell. A bsAb-mediated cross-linkage via CD3 leads to an activation of CD8+ T cells and consequently to killing of the target cells. In parallel, CD4+ T cells including TH1, TH2, TH17 cells and even regulatory T cells (Tregs) will be activated as well. Cytokines produced by CD4+ T cells can contribute to severe side effects e. g. life-threatening cytokine storms and, thinking of the immunosupressive function of Tregs, can even be counterproductive. Therefore, we asked whether or not it is feasible to limit retargeting to CD8+ T cells e. g. via targeting of the co-receptor CD8 instead of CD3. In order to test for proof of concept, a novel bsAb with specificity for CD8 and a tumor-associated surface antigen was constructed. Interestingly, we found that pre-activated (but not freshly isolated) CD8+ T cells can be retargeted via CD8-engaging bsAbs leading to an efficient lysis of target cells.

Published

2014

7. Proof of concept for a rapidly switchable universal CAR-T platform with UniCAR-T-CD123 in relapsed/refractory AML

Author

Michael Pehl, Sabrina Kraus, Gerhard Ehninger, Marc Cartellieri, Carla Kreissig, Malte von Bonin, Maria-Elisabeth Goebeler, Martin Wermke, Martin Bornhäuser, Ralf C. Bargou, Jan Moritz Middeke, Jan Koedam, Hermann Einsele, and Armin Ehninger

Subjects

Aged, 80 and over, Male, Oncology, medicine.medical_specialty, Receptors, Chimeric Antigen, business.industry, Immunology, Cell Biology, Hematology, Middle Aged, Immunotherapy, Adoptive, Proof of Concept Study, Biochemistry, Leukemia, Myeloid, Acute, Text mining, Proof of concept, Internal medicine, Relapsed refractory, Humans, Medicine, Car t cells, Letter to Blood, business, Aged

Published

2021

8. Rapidly Switchable Universal CAR-T Cells for Treatment of CD123-Positive Leukemia

Author

Jan-Erik Meyer, Simon Loff, Johannes Spehr, Marc Cartellieri, Mridula Swayampakula, Anja Feldmann, Armin Ehninger, Malte von Bonin, Gerhard Ehninger, Josephine Dietrich, Michael Bachmann, Cordula Gründer, Kristin Franke, and Julia Riewaldt

Subjects

0301 basic medicine, Cancer Research, Myeloid, medicine.medical_treatment, lcsh:RC254-282, Article, CD19, UniCAR, 03 medical and health sciences, 0302 clinical medicine, Antigen, AML, medicine, Pharmacology (medical), B cell, biology, adoptive cell therapy, Immunotherapy, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Chimeric antigen receptor, CAR-T, Haematopoiesis, Leukemia, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, CD123, biology.protein, Cancer research, Molecular Medicine, immunotherapy, ALL

Abstract

Chimeric antigen receptor T cells (CAR-T) targeting CD19 or B cell maturation antigen (BCMA) are highly effective against B cell malignancies. However, application of CAR-T to less differentially expressed targets remains a challenge due to lack of tumor-specific antigens and CAR-T controllability. CD123, a highly promising leukemia target, is expressed not only by leukemic and leukemia-initiating cells, but also by myeloid, hematopoietic progenitor, and certain endothelial cells. Thus, CAR-T lacking fine-tuned control mechanisms pose a high toxicity risk. To extend the CAR-T target landscape and widen the therapeutic window, we adapted our rapidly switchable universal CAR-T platform (UniCAR) to target CD123. UniCAR-T efficiently eradicated CD123+ leukemia in vitro and in vivo. Activation, cytolytic response, and cytokine release were strictly dependent on the presence of the CD123-specific targeting module (TM123) with comparable efficacy to CD123-specific CAR-T in vitro. We further demonstrated a pre-clinical proof of concept for the safety-switch mechanism using a hematotoxicity mouse model wherein TM123-redirected UniCAR-T showed reversible toxicity toward hematopoietic cells compared to CD123 CAR-T. In conclusion, UniCAR-T maintain full anti-leukemic efficacy, while ensuring rapid controllability to improve safety and versatility of CD123-directed immunotherapy. The safety and efficacy of UniCAR-T in combination with TM123 will now be assessed in a phase I clinical trial (ClinicalTrials.gov: NCT04230265)., Graphical Abstract, CAR-T cell treatment of acute leukemia beyond CD19 remains challenging. Loff et al. demonstrate that rapidly switchable universal CAR-T cells in combination with soluble CD123-specific adaptors achieve robust anti-leukemic responses, while hematotoxicity is rapidly reversible, enabling safe targeting of such less differentially expressed target antigens and broadening of the therapeutic window.

Published

2020

9. Phase 1 Dose Escalation Study of the Rapidly Switchable Universal CAR-T Therapy Unicar-T-CD123 in Relapsed/Refractory AML

Author

Gerhard Ehninger, Sabrina Kraus, Elisa Sala, Stephan K Metzelder, Vladan Vucinic, Walter Fiedler, Maria-Elisabeth Goebeler, Jan Moritz Middeke, Malte von Bonin, Carla Kreissig, Jan Koedam, Marc Cartellieri, Armin Ehninger, Martin Wermke, and Jonas A. Schäfer

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Published

2022

10. Chimeric antigen receptor T-cell therapy in acute myeloid leukemia

Author

Jan Koedam, Martin Wermke, Armin Ehninger, Marc Cartellieri, and Gerhard Ehninger

Subjects

Leukemia, Myeloid, Acute, Receptors, Chimeric Antigen, Cell- and Tissue-Based Therapy, Receptors, Antigen, T-Cell, Humans, Hematology, Immunotherapy, Adoptive

Abstract

Treatment outcome of relapsed or refractory AML patients remains dismal and new treatment options are needed. Adoptive cell therapy using CAR-T cells is a potentially interesting approach in this.Several potentially interesting AML targets are being investigated with CAR-T therapy with over 60 clinical trials listed on clinicaltrials.gov. The first clinical data are only just emerging with mixed results, once more proving that further research is needed.Adoptive cell therapy using chimeric antigen receptor T cells is being investigated in AML through many clinical trials. So far, no AML-specific antigen has been identified, requiring additional strategies to mitigate on-target off-tumor toxicity and to increase efficacy. Focus point is to acquire control over the CAR T cells once administered. Strategies to do so include biodegradable CARs, inducible CARs, suicide-switch containing CARs and two-component modular CARs. Limited and mixed results are available, confirming the risk of lasting toxicity for nonswitchable CARs. Initial results of modular CARs suggest toxicity can be mitigated whilst maintaining CAR activity by the use of modular CAR concepts that allows for 'ON' and 'OFF' switching.

Published

2022

11. Retargeting of UniCAR T cells with an in vivo synthesized target module directed against CD19 positive tumor cells

Author

Petra B. Welzel, Martin Bornhäuser, Roberta Aliperta, Gerhard Ehninger, Alexandra Kegler, Ralf Bergmann, Malte von Bonin, Stefanie Koristka, Carsten Werner, Armin Ehninger, Marc Cartellieri, Dominik Bachmann, Susann Albert, Anja Feldmann, Jörg Steinbach, Michael Bachmann, Simon Loff, Claudia Arndt, and Jens Pietzsch

Subjects

0301 basic medicine, biology, T cell, media_common.quotation_subject, Tumor cells, Art, University hospital, Virology, Chimeric antigen receptor, CD19, Epitope, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Oncology, Antigen, 030220 oncology & carcinogenesis, medicine, biology.protein, Tumor immunology, media_common

Abstract

// Dominik Bachmann 1 , Roberta Aliperta 1, * , Ralf Bergmann 2, * , Anja Feldmann 2, * , Stefanie Koristka 2, * , Claudia Arndt 2, * , Simon Loff 3, * , Petra Welzel 4 , Susann Albert 1 , Alexandra Kegler 2 , Armin Ehninger 3 , Marc Cartellieri 5 , Gerhard Ehninger 6, 7, 8 , Martin Bornhauser 6, 7, 8 , Malte von Bonin 6 , Carsten Werner 4 , Jens Pietzsch 2, 9 , Jorg Steinbach 2, 7, 8, 9 and Michael Bachmann 1, 2, 7, 8 1 University Cancer Center, Carl Gustav Carus TU Dresden, Tumor Immunology, Dresden, Germany 2 Helmholtz-Zentrum Dresden-Rossendorf, Institute of Radiopharmaceutical Cancer Research, Dresden, Germany 3 GEMoaB Monoclonals GmbH, Dresden, Germany 4 Leibniz Institute of Polymer Research Dresden, Dresden, Germany 5 Cellex Patient Treatment GmbH, Dresden, Germany 6 Medical Clinic and Policlinic I, University Hospital Carl Gustav Carus, TU Dresden, Dresden, Germany 7 German Cancer Consortium, Carl Gustav Carus TU Dresden, Dresden, Germany 8 National Center for Tumor Diseases, Dresden, Carl Gustav Carus TU Dresden, Dresden, Germany 9 Department of Chemistry and Food Chemistry, School of Science, TU Dresden, Dresden, Germany * These authors contributed equally to this work Correspondence to: Michael Bachmann, email: M.Bachmann@hzdr.de Keywords: CAR; CD19; retargeting; T cell; T cell therapy Received: October 09, 2017 Accepted: October 27, 2017 Published: December 21, 2017 ABSTRACT Recent treatments of leukemias with T cells expressing chimeric antigen receptors (CARs) underline their impressive therapeutic potential but also their risk of severe side effects including cytokine release storms and tumor lysis syndrome. In case of cross-reactivities, CAR T cells may also attack healthy tissues. To overcome these limitations, we previously established a switchable CAR platform technology termed UniCAR. UniCARs are not directed against typical tumor-associated antigens (TAAs) but instead against a unique peptide epitope: Fusion of this peptide epitope to a recombinant antibody domain results in a target module (TM). TMs can cross-link UniCAR T cells with tumor cells and thereby lead to their destruction. So far, we constructed TMs with a short half-life. The fast turnover of such a TM allows to rapidly interrupt the treatment in case severe side effects occur. After elimination of most of the tumor cells, however, longer lasting TMs which have not to be applied via continous infusion would be more convenient for the patient. Here we describe and characterize a TM for retargeting UniCAR T cells to CD19 positive tumor cells. Moreover, we show that the TM can efficiently be produced in vivo from producer cells housed in a sponge-like biomimetic cryogel and, thereby, serving as an in vivo TM factory for an extended retargeting of UniCAR T cells to CD19 positive leukemic cells.

Published

2017

12. Abstract 1506: Expansion kinetics and cytokine profiles of UniCAR-T-CD123, a rapidly switchable two-component CAR-T therapy, in patients with relapsed/refractory AML

Author

Marc Cartellieri, Carla Kreissig, Gerhard Ehninger, Jan Koedam, Armin Ehninger, Michael Pehl, Cordula Gründer, Kristin Franke, Julia Riewaldt, Sabrina Kraus, Martin Wermke, and Maria Schreiber

Subjects

Cancer Research, business.industry, Component (thermodynamics), medicine.medical_treatment, Kinetics, Cytokine, Oncology, Relapsed refractory, Cancer research, Medicine, In patient, Interleukin-3 receptor, Car t cells, business

Abstract

Background: Conventional CAR-T cells targeting CD123 in rrAML have achieved objective responses, but led to long-lasting myelosuppression due to expression of CD123 on progenitor cells. UniCAR-T-CD123 is a rapidly switchable two-component CAR-T therapy. An inert universal CAR-T cell (UniCAR-T) is combined with a CD123-specific soluble targeting module with a short half-life (TM123). By administering or withholding the continuous infusion of TM123, the UniCAR-T-cell can be rapidly switched on and off. Within the ongoing Phase IA study in rrAML, we investigated the expansion kinetics of UniCAR-T cells during TM123 administration in peripheral blood and bone marrow as well as cytokine profiles of treated patients. Methods: Prior to administration of autologous UniCAR-T cells, patients received a standard Flu/Cy lymphodepletion regimen at day -5 to -3. TM123 was administered as continuous infusion over 24 days starting at day 0. At day 1 a single dose of UniCAR-T cells was given. Dosing started with 1 x 108 UniCAR-T cells and 0.5 mg TM123 per day in patient 1. Patient 2 received the same TM123 dose and a UniCAR-T dose of 2.5 x 108 cells. Patient 3 received the same cell dose as patient 2 but a higher TM123 dose (1 mg/day). Pharmacokinetic of UniCAR-T and TM123 was determined from peripheral blood and bone marrow by droplet digital PCR and TM123-specific ELISA, respectively. Cytokine levels were measured by microfluidic immunoassay. Results: All 3 patients treated so far achieved an objective response, with one showing a PR and two a CRi. Treatment proved to be tolerable, no DLTs were observed to date and adverse events were mild. Grade 1 CRS (fever) was observed in 2 patients but subsided within 48 h after use of antipyretics. Myelosuppression was observed starting after lymphodepletion, which immediately recovered after TM123 withdrawal on day 24 in all patients, providing evidence for the rapid off-switch of UniCAR-T cells post TM123 administration. UniCAR-T cells expanded in all patients in peripheral blood and bone marrow comparable to data reported for conventional CD123 CAR-T products, and were so far detectable for up to 6 months after administration. Expansion kinetics were TM123-dependent. Patients showed periods of transient increase of IL-6, IFN-γ and TNF-α levels preceding peak expansion and decreasing after termination of TM123 administration. One patient showed additional coinciding momentary elevation of GM-CSF and IL-2. Conclusions: The initial clinical and translational results of UniCAR-T-CD123 represent, to our understanding, a first time evidence for a well-tolerated and effective rapidly switchable CAR-T product. Even though the number of patients treated so far is limited, the data obtained provide clinical proof-of-concept for the opportunity to abrogate side effects by withdrawal of TM123. Enrollment into the Phase IA study is ongoing. Citation Format: Armin Ehninger, Julia Riewaldt, Cordula Gründer, Kristin Franke, Maria Schreiber, Martin Wermke, Sabrina Kraus, Carla Kreissig, Jan Koedam, Michael Pehl, Gerhard Ehninger, Marc Cartellieri. Expansion kinetics and cytokine profiles of UniCAR-T-CD123, a rapidly switchable two-component CAR-T therapy, in patients with relapsed/refractory AML [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 1506.

Published

2021

13. Abstract 2209: Rapidly switchable universal CAR-T cells with improved safety profile allow for active targeting of PD-L1 expressing solid tumors

Author

Gerhard Ehninger, Marc Cartellieri, Josephine Dietrich, Michael Pehl, Johannes Spehr, Simon Loff, Cordula Gründer, Julia Riewaldt, Armin Ehninger, Maria Schreiber, and Michael Bachmann

Subjects

Cancer Research, Safety profile, Oncology, biology, Chemistry, PD-L1, biology.protein, Cancer research, Car t cells

Abstract

Despite remarkable therapeutic success using chimeric antigen receptor modified T-cells (CAR-T) in hematologic malignancies, targeting solid tumors still remains challenging, given their heterogeneity and immunosuppressive milieu, including the expression of inhibitory immune checkpoints such as PD-1/PD-L1. Preclinical models demonstrate that combining CAR-T therapy with checkpoint inhibitors targeting the PD-1/PD-L1 axis could be a promising strategy to enhance anti-cancer activity of CAR-T in solid tumors and on-going phase I trials are clinically evaluating this strategy. However, primary and acquired resistance to checkpoint blockade is frequently observed limiting its broad applicability and efficacy. In addition, lack of specificity results in frequent occurrence of immune-related adverse events affecting several organs. Alternatively, expression of PD-L1 by solid tumor cells could be an attractive target for CAR-T therapy, especially in order to prevent or reverse tumor re-growth and relapse after successful initial tumor cell lysis. The development of a rapidly switchable universal CAR-T platform (UniCAR) with enhanced safety features allowed us to explore the possibility to directly attack PD-L1 expressing solid tumor cells. An inherent key feature of the UniCAR-T platform is a rapid and reversible turn off mechanism (less than 4 hours) determined by the short pharmacokinetic half-life of soluble targeting modules (TMs) and fast internalization of cell-bound TMs. TMs provide the antigen-specificity for UniCAR gene-modified T-cells (UniCAR-T) and consist of an antigen-binding moiety, e.g. an scFv, linked to a small peptide motif recognized by the UniCAR. For redirecting UniCAR-T against the PD-1/PD-L1 axis, a PD-L1 specific TM (TM-PD-L1) was developed and its functionality confirmed in binding assays to human and murine PD-L1 using surface plasmon resonance as well as in cell-based cytotoxicity assays. Half maximal killing efficacy (EC50) mediated by TM-PD-L1 redirected UniCAR-T was in the low picomolar range. As PD-L1 is also expressed on healthy tissue, toxicity studies were performed in a humanized mouse model with human UniCAR-T. Humanized mice treated with TM-PD-L1 twice a day for ten consecutive days did not reveal any signs of toxicity. In a prostate cancer (PCa) xenograft model efficient suppression of tumor growth could be demonstrated by administration of TM-PD-L1. Our data are the first to demonstrate safety and feasibility of active targeting of PD-L1 expressed by solid tumors with CAR-T and that this approach is capable of inducing a significant anti-tumor response. Citation Format: Josephine Dietrich, Simon Loff, Johannes Spehr, Julia Riewaldt, Cordula Gründer, Maria Schreiber, Michael Bachmann, Gerhard Ehninger, Michael Pehl, Marc Cartellieri, Armin Ehninger. Rapidly switchable universal CAR-T cells with improved safety profile allow for active targeting of PD-L1 expressing solid tumors [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 2209.

Published

2020

14. Abstract 2176: Using a PSMA-specific low-molecular-weight compound for prostate cancer treatment with rapidly switchable universal CAR-T cells: Overcoming the challenges of cellular immunotherapies in solid tumors

Author

Simon Loff, Gerhard Ehninger, Mridula Swayampakula, Michael Pehl, Maria Schreiber, Julia Riewaldt, Armin Ehninger, Anja Feldmann, Cordula Gründer, Marc Cartellieri, Michael Bachmann, and Johannes Spehr

Subjects

Cancer Research, business.industry, Normal tissue, Tumor penetration, CD28, Cancer, medicine.disease, Cell therapy, Prostate cancer, Oncology, medicine, Cancer research, Car t cells, business

Abstract

CAR-T cell therapy holds great promise for treating a wide range of malignancies. Nevertheless, the CAR-T approach faces multiple challenges, including lack of suitable targets, insufficient tumor penetration and a microenvironment hostile to CAR-T cells. Here we provide pre-clinical evidence for using a low-molecular-weight, chemically synthesized compound to re-target CAR-T cells against solid tumors in conjunction with the CD28 co-stimulatory domain to address several of these challenges. PSMA is a validated target for treatment of advanced and metastatic prostate cancer (PCa), but also broadly expressed on tumor neo-vasculature beyond PCa. PSMA is also known to be expressed on a number of normal tissues, albeit to a much lower extent, which necessitates additional safety mechanisms for CAR-T therapy. Therefore, a rapidly switchable universal CAR-T platform (UniCAR) was developed. In this system, antigen-specificity is provided by soluble adaptors termed targeting modules (TM), which redirect T-cells engineered to express a universal CAR in an antigen-specific manner against tumors. The TM explored in the present study incorporates a clinically well-characterized radiotracer peptide motif binding to the enzymatic groove of PSMA. The small-sized TM has favorable pharmacokinetic and pharmacodynamics properties (short half-life of < 30 min; rapid internalization in < 1h), which allows a fast silencing and excellent controllability of UniCAR-T reactivity (< 4 h). Furthermore, the small molecule TM efficiently penetrates and rapidly accumulates within solid tumors as clinically demonstrated by related radiotracers. Results from our pre-clinical in vivo model demonstrate potent recruitment of UniCAR-T into tumor tissue by the TM and an efficient anti-tumor response. Of note, it was recently shown that the chosen PCa model suppresses CAR-T response by secreting high levels of transforming growth factor beta (TGF-β), creating an immunosuppressive milieu. We could overcome immunosuppression utilizing CD28 compared to 4-1-BB in the intracellular signaling domain of the UniCAR. Administered CD28/zeta UniCAR efficiently suppressed tumor growth in our in vivo model and could be re-activated by consecutive cycles of TM administration even after several weeks. In contrast to CARs with fixed binding moieties, which continuously signal and thereby induce T- cell exhaustion, the discontinuous activation of UniCAR keeps a balanced mix of T-effector and T-memory cells. In summary, our rapidly switchable universal CAR-T platform in combination with a low-molecular-weight TM allows to target less differentially expressed solid tumor antigens. Furthermore, incorporation of the CD28 costimulatory domain overcomes the immunosuppressive tumor microenvironment while discontinuous activation of UniCAR-T prevents exhaustion. Citation Format: Marc Cartellieri, Simon Loff, Johannes Spehr, Mridula Swayampakula, Julia Riewaldt, Cordula Gründer, Maria Schreiber, Michael Bachmann, Anja Feldmann, Michael Pehl, Gerhard Ehninger, Armin Ehninger. Using a PSMA-specific low-molecular-weight compound for prostate cancer treatment with rapidly switchable universal CAR-T cells: Overcoming the challenges of cellular immunotherapies in solid tumors [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 2176.

Published

2020

15. Abstract 4232: More than a bridging therapy: Targeting CD123 with rapidly switchable universal CAR-T cells for treatment of acute leukemia

Author

Jan-Erik Meyer, Marc Cartellieri, Johannes Spehr, Maria Schreiber, Gerhard Ehninger, Michael Pehl, Michael Bachmann, Simon Loff, Armin Ehninger, Cordula Gründer, and Julia Riewaldt

Subjects

Cancer Research, Acute leukemia, biology, business.industry, CD19, Chimeric antigen receptor, Haematopoiesis, Oncology, Antigen, In vivo, Cancer research, biology.protein, Medicine, Interleukin-3 receptor, Progenitor cell, business

Abstract

Chimeric antigen receptor T-cell (CAR-T) therapy targeting CD19 or BCMA is tremendously effective in treating hematological malignancies. However, the application of CAR-T beyond certain B-cell malignancies such as ALL, MM, lymphoma and CLL remains challenging due to the lack of tumor-specific antigens and the limited ability to control acute and potential long term CAR-T reactivity in patients. Therefore, a rapidly switchable universal CAR-T platform (UniCAR) was developed. In this system, antigen-specificity is provided by soluble adaptors of short pharmacokinetic half-life, termed targeting modules (TM), which redirect T-cells engineered to express a universal CAR against tumors, allowing for excellent controllability of CAR-T reactivity while maintaining the high anti-tumor activity of CAR-T cells. Here we present results from late stage pre-clinical characterization of UniCAR-T targeting CD123 (UniCAR-T-CD123) for treatment of acute leukemia. Pre-clinical characterization confirmed specificity and safety of the approach. UniCAR-T proofed to be per se inert and safe in clinically relevant in vivo toxicity models. Activation of UniCAR-T occurs solely in the presence of the CD123-specific TM (TM123) and upon cross-linkage to CD123 expressing leukemic cells. Specific lysis of leukemic target cell lines and primary patient material is induced in a dose-dependent manner at pico-molar TM123 concentrations. Notably, induction of cytokine release occurs at higher TM doses than on-set of target cell lysis, opening a therapeutic window for clinical application. In vivo efficacy of UniCAR-T re-directed against CD123 was proven in CDX and PDX mouse models. Interestingly, anti-leukemic responses of switch-controllable UniCAR-T were demonstrated to be comparable to conventional CD123-specific CAR-T in vitro at comparable doses. In contrast to conventional CD123 CAR-T, CD123-specific toxicity of TM-activated UniCAR-T towards hematopoietic progenitors was reversible and could be abrogated by withdrawal of TM, allowing for normal development of human hematopoiesis in a xenograft model. In summary, in vitro and in vivo evidence suggests that UniCAR-T-CD123 could provide strong efficacy against CD123 expressing hematological malignancies while providing excellent control and ensuring recovery of normal hematopoiesis post treatment. A phase IA dose-finding study is ongoing. Citation Format: Simon Loff, Jan-Erik Meyer, Johannes Spehr, Julia Riewaldt, Cordula Gründer, Maria Schreiber, Michael Bachmann, Michael Pehl, Gerhard Ehninger, Armin Ehninger, Marc Cartellieri. More than a bridging therapy: Targeting CD123 with rapidly switchable universal CAR-T cells for treatment of acute leukemia [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 4232.

Published

2020

16. Tonic Signaling and Its Effects on Lymphopoiesis of CAR-Armed Hematopoietic Stem and Progenitor Cells

Author

Michael Bachmann, Martin Bornhäuser, Alexander Gerbaulet, Anja Feldmann, Anne Eugster, Gerhard Ehninger, Ezio Bonifacio, Nicole Berndt, Susann Albert, Claudia Arndt, Liliana R. Loureiro, Malte von Bonin, Stefanie Koristka, Marc Cartellieri, and Armin Ehninger

Subjects

Adoptive cell transfer, Immunology, Biology, Lymphocyte Activation, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, medicine, Immunology and Allergy, Animals, Humans, Lymphopoiesis, Progenitor cell, Receptors, Chimeric Antigen, Hematopoietic Stem Cell Transplantation, Cell Differentiation, Hematopoietic Stem Cells, Adoptive Transfer, Cell biology, Transplantation, Mice, Inbred C57BL, Haematopoiesis, medicine.anatomical_structure, Bone marrow, Stem cell, human activities, 030215 immunology, Signal Transduction

Abstract

Long-term survival of adoptively transferred chimeric Ag receptor (CAR) T cells is often limited. Transplantation of hematopoietic stem cells (HSCs) transduced to express CARs could help to overcome this problem as CAR-armed HSCs can continuously deliver CAR+ multicell lineages (e.g., T cells, NK cells). In dependence on the CAR construct, a variable extent of tonic signaling in CAR T cells was reported; thus, effects of CAR-mediated tonic signaling on the hematopoiesis of CAR-armed HSCs is unclear. To assess the effects of tonic signaling, two CAR constructs were established and analyzed 1) a signaling CAR inducing a solid Ag-independent tonic signaling termed CAR-28/ζ and 2) a nonstimulating control CAR construct lacking intracellular signaling domains termed CAR-Stop. Bone marrow cells from immunocompetent mice were isolated, purified for HSC-containing Lin−cKit+ cells or the Lin−cKit+ Sca-1+ subpopulation (Lin−Sca-1+cKit+), and transduced with both CAR constructs. Subsequently, modified bone marrow cells were transferred into irradiated mice, in which they successfully engrafted and differentiated into hematopoietic progenitors. HSCs expressing the CAR-Stop sustained normal hematopoiesis. In contrast, expression of the CAR-28/ζ led to elimination of mature CAR+ T and B cells, suggesting that the CAR-mediated tonic signaling mimics autorecognition via the newly recombined immune receptors in the developing lymphocytes.

Published

2018

17. Engrafting human regulatory T cells with a flexible modular chimeric antigen receptor technology

Author

Marc Schmitz, Michael Bachmann, Marc Cartellieri, Martin Bornhäuser, Ralf Bergmann, Jan Moritz Middeke, Katja Akgün, Jörg Steinbach, Susann Albert, Alexandra Kegler, Armin Ehninger, Anja Feldmann, Stefanie Koristka, Gerhard Ehninger, Claudia Arndt, Jens Pietzsch, and Tjalf Ziemssen

Subjects

0301 basic medicine, Adoptive cell transfer, CD28, medicine.medical_treatment, CD137 (4-1BB), Immunology, Receptors, Antigen, T-Cell, chemical and pharmacologic phenomena, T-Cell Antigen Receptor Specificity, Biology, Immunotherapy, Adoptive, T-Lymphocytes, Regulatory, regulatory T cells, 03 medical and health sciences, Mice, Tumor Necrosis Factor Receptor Superfamily, Member 9, medicine, Immunology and Allergy, Animals, Humans, Cells, Cultured, Receptors, Chimeric Antigen, chimeric antigen receptor, Effector, CD137, hemic and immune systems, Immunotherapy, Adoptive Transfer, Chimeric antigen receptor, Cell biology, Tolerance induction, Receptors, Antigen, 030104 developmental biology, HEK293 Cells, NIH 3T3 Cells, immunotherapy, Function (biology)

Abstract

As regulatory T cells (Tregs) play a fundamental role in immune homeostasis their adoptive transfer emerged as a promising treatment strategy for inflammation-related diseases. Preclinical animal models underline the superiority of antigen-specific Tregs compared to polyclonal cells. Here, we applied a modular chimeric antigen receptor (CAR) technology called UniCAR for generation of antigen-specific human Tregs. In contrast to conventional CARs, UniCAR-endowed Tregs are indirectly linked to their target cells via a separate targeting module (TM). Thus, transduced Tregs can be applied universally as their antigen-specificity is easily adjusted by TM exchange. Activation of UniCAR-engrafted Tregs occurred in strict dependence on the TM, facilitating a precise control over Treg activity. In order to augment efficacy and safety, different intracellular signaling domains were tested. Both 4-1BB (CD137) and CD28 costimulation induced strong suppressive function of genetically modified Tregs. However, in light of safety issues, UniCARs comprising a CD137-CD3ζ signaling domain emerged as constructs of choice for a clinical application of redirected Tregs. In that regard, Tregs isolated from patients suffering from autoimmune or inflammatory diseases were, for the first time, successfully engineered with UniCAR 137/ζ and efficiently suppressed patient-derived effector cells. Overall, the UniCAR platform represents a promising approach to improve Treg-based immunotherapies for tolerance induction.

Published

2017

18. Retargeting of UniCAR T cells with an

Author

Dominik, Bachmann, Roberta, Aliperta, Ralf, Bergmann, Anja, Feldmann, Stefanie, Koristka, Claudia, Arndt, Simon, Loff, Petra, Welzel, Susann, Albert, Alexandra, Kegler, Armin, Ehninger, Marc, Cartellieri, Gerhard, Ehninger, Martin, Bornhäuser, Malte, von Bonin, Carsten, Werner, Jens, Pietzsch, Jörg, Steinbach, and Michael, Bachmann

Subjects

CD19, T cell therapy, T cell, Research Paper, CAR, retargeting

Abstract

Recent treatments of leukemias with T cells expressing chimeric antigen receptors (CARs) underline their impressive therapeutic potential but also their risk of severe side effects including cytokine release storms and tumor lysis syndrome. In case of cross-reactivities, CAR T cells may also attack healthy tissues. To overcome these limitations, we previously established a switchable CAR platform technology termed UniCAR. UniCARs are not directed against typical tumor-associated antigens (TAAs) but instead against a unique peptide epitope: Fusion of this peptide epitope to a recombinant antibody domain results in a target module (TM). TMs can cross-link UniCAR T cells with tumor cells and thereby lead to their destruction. So far, we constructed TMs with a short half-life. The fast turnover of such a TM allows to rapidly interrupt the treatment in case severe side effects occur. After elimination of most of the tumor cells, however, longer lasting TMs which have not to be applied via continous infusion would be more convenient for the patient. Here we describe and characterize a TM for retargeting UniCAR T cells to CD19 positive tumor cells. Moreover, we show that the TM can efficiently be produced in vivo from producer cells housed in a sponge-like biomimetic cryogel and, thereby, serving as an in vivo TM factory for an extended retargeting of UniCAR T cells to CD19 positive leukemic cells.

Published

2017

19. Development of novel target modules for retargeting of UniCAR T cells to GD2 positive tumor cells

Author

Nicola, Mitwasi, Anja, Feldmann, Ralf, Bergmann, Nicole, Berndt, Claudia, Arndt, Stefanie, Koristka, Alexandra, Kegler, Justyna, Jureczek, Anja, Hoffmann, Armin, Ehninger, Marc, Cartellieri, Susann, Albert, Claudia, Rossig, Gerhard, Ehninger, Jens, Pietzsch, Jörg, Steinbach, and Michael, Bachmann

Subjects

CAR T cells, immunotherapy, Research Paper

Abstract

As the expression of a tumor associated antigen (TAA) is commonly not restricted to tumor cells, adoptively transferred T cells modified to express a conventional chimeric antigen receptor (CAR) might not only destroy the tumor cells but also attack target-positive healthy tissues. Furthermore, CAR T cells in patients with large tumor bulks will unpredictably proliferate and put the patients at high risk of adverse side effects including cytokine storms and tumor lysis syndrome. To overcome these problems, we previously established a modular CAR technology termed UniCAR: UniCAR T cells can repeatedly be turned on and off via dosing of a target module (TM). TMs are bispecific molecules which cross-link UniCAR T cells with target cells. After elimination of the respective TM, UniCAR T cells automatically turn off. Here we describe novel TMs against the disialoganglioside GD2 which is overexpressed in neuroectodermal but also many other tumors. In the presence of GD2-specific TMs, we see a highly efficient target-specific and -dependent activation of UniCAR T cells, secretion of pro-inflammatory cytokines, and tumor cell lysis both in vitro and experimental mice. According to PET-imaging, anti-GD2 TM enrich at the tumor site and are rapidly eliminated thus fulfilling all prerequisites of a UniCAR TM.

Published

2017

20. Simultaneous targeting of prostate stem cell antigen and prostate-specific membrane antigen improves the killing of prostate cancer cells using a novel modular T cell-retargeting system

Author

Maria Dimmel, Marc Cartellieri, Anja Feldmann, Gerhard Ehninger, Claudia Arndt, Armin Ehninger, Stefanie Koristka, and Michael Bachmann

Subjects

Urology, medicine.medical_treatment, T cell, Immunotherapy, Biology, medicine.disease, Molecular biology, Prostate Stem Cell Antigen, Prostate cancer, medicine.anatomical_structure, Oncology, Tumor Escape, Antigen, Prostate, medicine, Glutamate carboxypeptidase II, Cancer research

Abstract

BACKGROUND Recently, we described a novel modular platform technology in which T cell-recruitment and tumor-targeting domains of conventional bispecific antibodies are split to independent components, a universal effector module (EM) and replaceable monospecific/monovalent target modules (TMs) that form highly efficient T cell-retargeting complexes. Theoretically, our unique strategy should allow us to simultaneously retarget T cells to different tumor antigens by combining the EM with two or more different monovalent/monospecific TMs or even with bivalent/bispecific TMs, thereby overcoming limitations of a monospecific treatment such as the selection of target-negative tumor escape variants. METHODS In order to advance our recently introduced prostate stem cell antigen (PSCA)-specific modular system for a dual-targeting of prostate cancer cells, two additional TMs were constructed: a monovalent/monospecific TM directed against the prostate-specific membrane antigen (PSMA) and a bivalent/bispecific TM (bsTM) with specificity for PSMA and PSCA. The functionality of the novel dual-targeting strategies was analyzed by performing T cell activation and chromium release assays. RESULTS Similar to the PSCA-specific modular system, the novel PSMA-specific modular system mediates an efficient target-dependent and -specific tumor cell lysis at low E:T ratios and picomolar Ab concentrations. Moreover, by combination of the EM with either the bispecific TM directed to PSMA and PSCA or both monospecifc TMs directed to either PSCA or PSMA, dual-specific targeting complexes were formed which allowed us to kill potential escape variants expressing only one or the other target antigen. CONCLUSIONS Overall, the novel modular system represents a promising tool for multiple tumor targeting. Prostate 74: 1335–1346, 2014. © 2014 Wiley Periodicals, Inc.

Published

2014

21. Redirection of CD4+ and CD8+ T lymphocytes via a novel antibody-based modular targeting system triggers efficient killing of PSCA+ prostate tumor cells

Author

Armin Ehninger, Marc Cartellieri, Achim Temme, Katrin Töpfer, Gerhard Ehninger, Michael Bachmann, Anja Feldmann, Claudia Arndt, and Stefanie Koristka

Subjects

biology, Urology, medicine.medical_treatment, T cell, Immunotherapy, medicine.disease, Prostate Stem Cell Antigen, Prostate cancer, medicine.anatomical_structure, Oncology, Antigen, In vivo, Immunology, biology.protein, medicine, Cancer research, Antibody, CD8

Abstract

BACKGROUND There is still a need for new therapeutic options against prostate cancer. Conventional single-chain bispecific antibodies (bsAbs), that directly cross-link T cells and tumor cells, hold great potential for efficient tumor treatment. However, rapid development of novel bsAbs is hampered by laborious optimization to improve their efficacy and reduce potential side effects. To accelerate the development of a novel antibody tool for the redirection of T cells to different tumor-associated antigens, we recently introduced a modular targeting system. METHODS We here describe a novel modular system for treatment of prostate cancer by retargeting of T cells to the prostate stem cell antigen (PSCA). Functionality of the novel PSCA-specific modular system was investigated in vitro by T cell activation and chromium release assays as well as in immunodeficient mice. RESULTS Similar to a conventional bsAb CD3-PSCA, the novel PSCA-specific modular system induces activation of both CD4+ and CD8+ T cells leading to secretion of pro-inflammatory cytokines and highly efficient target-specific tumor cell lysis. The novel TM was ready-to-use from the time point of construction and functional at low E:T ratios and picomolar concentrations without further optimization. In addition, the PSCA-specific modular system delays outgrowth of s.c. tumors in mice comparable to bsAb CD3-PSCA. CONCLUSIONS We have developed a novel PSCA-specific modular system which triggers an efficient T cell-mediated killing of PSCA+ tumor cells in vitro and in vivo. The new Ab-based targeting strategy can functionally replace conventional bsAbs and allows a flexible redirection of T cells to different tumor-associated antigens. Prostate 74: 1347–1358, 2014. © 2014 Wiley Periodicals, Inc.

Published

2014

22. Loss of SPARC protects hematopoietic stem cells from chemotherapy toxicity by accelerating their return to quiescence

Author

Katja Müdder, Armin Ehninger, Gertraud Orend, Andreas Trumpp, Tobias Boch, and Hind Medyouf

Subjects

Antimetabolites, Antineoplastic, medicine.medical_treatment, Immunology, Hematopoietic stem cell transplantation, Biology, Biochemistry, Extracellular matrix, Mice, Extracellular, medicine, Animals, Osteonectin, Mice, Knockout, Transplantation Chimera, Fetus, Hematopoietic Stem Cell Transplantation, Cell Biology, Hematology, Allografts, Hematopoietic Stem Cells, Cell biology, Haematopoiesis, medicine.anatomical_structure, Cellular Microenvironment, Toxicity, Fluorouracil, Bone marrow, Stem cell

Abstract

Around birth, hematopoietic stem cells (HSCs) expanding in the fetal liver migrate to the developing bone marrow (BM) to mature and expand. To identify the molecular processes associated with HSCs located in the 2 different microenvironments, we compared the expression profiles of HSCs present in the liver and BM of perinatal mice. This revealed the higher expression of a cluster of extracellular matrix-related genes in BM HSCs, with secreted protein acidic and rich in cysteine (SPARC) being one of the most significant ones. This extracellular matrix protein has been described to be involved in tissue development, repair, and remodeling, as well as metastasis formation. Here we demonstrate that SPARC-deficient mice display higher resistance to serial treatment with the chemotherapeutic agent 5-fluorouracil (5-FU). Using straight and reverse chimeras, we further show that this protective effect is not due to a role of SPARC in HSCs, but rather is due to its function in the BM niche. Although the kinetics of recovery of the hematopoietic system is normal, HSCs in a SPARC-deficient niche show an accelerated return to quiescence, protecting them from the lethal effects of serial 5-FU treatment. This may become clinically relevant, as SPARC inhibition and its protective effect on HSCs could be used to optimize chemotherapy schemes.

Published

2014

23. Clinical-grade manufacturing of switchable CAR-T cells in an automated closed system for phase I/II trials

Author

Julia Riewaldt, Josephine Dietrich, Simon Loff, Cordula Gründer, G. Ehninger, K. Franke, Jan-Erik Meyer, S. Schallenberg, Michael Bachmann, C. Kreissig, Marc Cartellieri, Armin Ehninger, and Johannes Spehr

Subjects

Cancer Research, Transplantation, Phase i ii, Oncology, Computer science, Control theory, Closed system, Immunology, Immunology and Allergy, Clinical grade, Cell Biology, Car t cells, Genetics (clinical)

Published

2018

24. Characterization of a switchable chimeric antigen receptor platform in a pre-clinical solid tumor model

Author

Elham Pishali Bejestani, Anja Feldmann, Gerhard Ehninger, Ralf Bergmann, Mechthild Krause, Marc Cartellieri, Susann Albert, Johannes Spehr, Malte von Bonin, Michael Baumann, Antje Dietrich, Simon Loff, Martin Wermke, Martin Bornhäuser, Michael Bachmann, Armin Ehninger, and Michael Kramer

Subjects

0301 basic medicine, lcsh:Immunologic diseases. Allergy, Immunology, Biology, lcsh:RC254-282, 03 medical and health sciences, Prostate cancer, Downregulation and upregulation, In vivo, medicine, Immunology and Allergy, Original Research, immune checkpoints, solid tumors, medicine.disease, chimeric antigen receptors, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Molecular biology, Chimeric antigen receptor, In vitro, Prostate Stem Cell Antigen, 030104 developmental biology, Oncology, targeting module, prostate stem cell antigen, Cancer cell, Chimeric antigen receptors, Cancer research, immunoevasion, Cell activation, lcsh:RC581-607

Abstract

The universal modular chimeric antigen receptor (UniCAR) platform redirects CAR-T cells using a separated, soluble targeting module with a short half-life. This segregation allows precise controllability and flexibility. Herein we show that the UniCAR platform can be used to efficiently target solid cancers in vitro and in vivo using a pre-clinical prostate cancer model which overexpresses prostate stem cell antigen (PSCA). Short-term administration of the targeting module to tumor bearing immunocompromised mice engrafted with human UniCAR-T cells significantly delayed tumor growth and prolonged survival of recipient mice both in a low and high tumor burden model. In addition, we analyzed phenotypic and functional changes of cancer cells and UniCAR-T cells in association with the administration of the targeting module to reveal potential immunoevasive mechanisms. Most notably, UniCAR-T cell activation induced upregulation of immune-inhibitory molecules such as programmed death ligands. In conclusion, this work illustrates that the UniCAR platform mediates potent anti-tumor activity in a relevant in vitro and in vivo solid tumor model.

Published

2016

25. A novel nanobody-based target module for retargeting of T lymphocytes to EGFR-expressing cancer cells via the modular UniCAR platform

Author

Jörg Steinbach, Florian Ludwig, Jens Pietzsch, Sebastian Gärtner, Michael Bachmann, Gerhard Ehninger, Dominik Bachmann, Susann Albert, Claudia Arndt, Hans-Jürgen Pietzsch, Pauline Ziller-Walter, Ralf Bergmann, Stefanie Koristka, Marc Cartellieri, Alexandra Kegler, Anja Feldmann, Marc Schmitz, and Armin Ehninger

Subjects

0301 basic medicine, lcsh:Immunologic diseases. Allergy, Retargeting, EGFR, T cell, Immunology, Peptide, lcsh:RC254-282, Epitope, car, law.invention, t cell therapy, 03 medical and health sciences, 0302 clinical medicine, law, medicine, Immunology and Allergy, Receptor, retargeting, Original Research, chemistry.chemical_classification, Chemistry, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, t cell, Chimeric antigen receptor, CAR, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, T cell therapy, Cancer cell, egfr, Recombinant DNA, lcsh:RC581-607

Abstract

Recent treatments of leukemias with chimeric antigen receptor (CAR) expressing T cells underline their impressive therapeutic potential. However, once adoptively transferred into patients, there is little scope left to shut them down after elimination of tumor cells or in case adverse side effects occur. This becomes of special relevance if they are directed against commonly expressed tumor associated antigens (TAAs) such as receptors of the ErbB family. To overcome this limitation, we recently established a modular CAR platform technology termed UniCAR. UniCARs are not directed against TAAs but instead against a unique peptide epitope on engineered recombinant targeting modules (TMs), which guide them to the target. In the absence of a TM UniCAR T cells are inactive. Thus an interruption of any UniCAR activity requires an elimination of unbound TM and the TM complexed with UniCAR T cells. Elimination of the latter one requires a disassembly of the UniCAR-TM complexes. Here, we describe a first nanobody (nb)-based TM directed against EGFR. The novel TM efficiently retargets UniCAR T cells to EGFR positive tumors and mediates highly efficient target-specific and target-dependent tumor cell lysis both in vitro and in vivo. After radiolabeling of the novel TM with 64Cu and 68Ga, we analyzed its biodistribution and clearance as well as the stability of the UniCAR-TM complexes. As expected unbound TM is rapidly eliminated while the elimination of the TM complexed with UniCAR T cells is delayed. Nonetheless, we show that UniCAR-TM complexes dissociate in vitro and in vivo in a concentration-dependent manner in line with the concept of a repeated stop and go retargeting of tumor cells via the UniCAR technology.

Published

2016

26. Retargeting of T lymphocytes to PSCA- or PSMA positive prostate cancer cells using the novel modular chimeric antigen receptor platform technology 'UniCAR'

Author

Anja, Feldmann, Claudia, Arndt, Ralf, Bergmann, Simon, Loff, Marc, Cartellieri, Dominik, Bachmann, Roberta, Aliperta, Mirjam, Hetzenecker, Florian, Ludwig, Susann, Albert, Pauline, Ziller-Walter, Alexandra, Kegler, Stefanie, Koristka, Sebastian, Gärtner, Marc, Schmitz, Armin, Ehninger, Gerhard, Ehninger, Jens, Pietzsch, Jörg, Steinbach, and Michael, Bachmann

Subjects

Cytotoxicity, Immunologic, Male, Recombinant Fusion Proteins, T-Lymphocytes, Genetic Vectors, Receptors, Antigen, T-Cell, T cells, Prostatic Neoplasms, T-Cell Antigen Receptor Specificity, GPI-Linked Proteins, Lymphocyte Activation, Xenograft Model Antitumor Assays, Neoplasm Proteins, CAR, Disease Models, Animal, Mice, Antigens, Neoplasm, Cell Line, Tumor, Leukocytes, Mononuclear, Animals, Cytokines, Humans, Immunotherapy, Research Paper, retargeting

Abstract

New treatment options especially of solid tumors including for metastasized prostate cancer (PCa) are urgently needed. Recent treatments of leukemias with chimeric antigen receptors (CARs) underline their impressive therapeutic potential. However CARs currently applied in the clinics cannot be repeatedly turned on and off potentially leading to severe life threatening side effects. To overcome these problems, we recently described a modular CAR technology termed UniCAR: UniCAR T cells are inert but can be turned on by application of one or multiple target modules (TMs). Here we present preclinical data summarizing the retargeting of UniCAR T cells to PCa cells using TMs directed to prostate stem cell- (PSCA) or/and prostate specific membrane antigen (PSMA). In the presence of the respective TM(s), we see a highly efficient target-specific and target-dependent activation of UniCAR T cells, secretion of pro-inflammatory cytokines, and PCa cell lysis both in vitro and experimental mice.

Published

2016

27. The bone marrow stem cell niche grows up: mesenchymal stem cells and macrophages move in (Review)

Author

Armin Ehninger and Andreas Trumpp

Subjects

Immunology, Clinical uses of mesenchymal stem cells, Stem cell factor, Review, Biology, Monocytes, 03 medical and health sciences, 0302 clinical medicine, Cancer stem cell, Bone Marrow, Granulocyte Colony-Stimulating Factor, Immunology and Allergy, Animals, Humans, Progenitor cell, Stem Cell Niche, 030304 developmental biology, Stem cell transplantation for articular cartilage repair, 0303 health sciences, Macrophages, Bone Marrow Stem Cell, Mesenchymal Stem Cells, Cell biology, 030220 oncology & carcinogenesis, Stem cell, Adult stem cell

Abstract

Ehninger and Trumpp discuss the role of monocytes/macrophages and other niche cells in the regulation of HSC mobilization and retention., Stem cell niches are defined as the cellular and molecular microenvironments that regulate stem cell function together with stem cell autonomous mechanisms. This includes control of the balance between quiescence, self-renewal, and differentiation, as well as the engagement of specific programs in response to stress. In mammals, the best understood niche is that harboring bone marrow hematopoietic stem cells (HSCs). Recent studies have expanded the number of cell types contributing to the HSC niche. Perivascular mesenchymal stem cells and macrophages now join the previously identified sinusoidal endothelial cells, sympathetic nerve fibers, and cells of the osteoblastic lineage to form similar, but distinct, niches that harbor dormant and self-renewing HSCs during homeostasis and mediate stem cell mobilization in response to granulocyte colony-stimulating factor.

Published

2011

28. Late-Stage Preclinical Characterization of Switchable CD123-Specific CAR-T for Treatment of Acute Leukemia

Author

Jan-Erik Meyer, Gerhard Ehninger, Josephine Dietrich, Riewaldt Julia, Kristin Franke, Anja Feldmann, Michael Bachmann, Armin Ehninger, Simon Loff, Cordula Gründer, Marc Cartellieri, Johannes Spehr, and Malte von Bonin

Subjects

0301 basic medicine, biology, business.industry, Immunology, Cell Biology, Hematology, Biochemistry, Chimeric antigen receptor, CD19, Transplantation, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Lymphocyte costimulation, Cancer research, biology.protein, Medicine, Chimeric Antigen Receptor T-Cell Therapy, Stem cell, Progenitor cell, business, B cell

Abstract

Application of autologous T cells genetically engineered to express CD19-specific chimeric antigen receptors (CAR-T) is highly effective in the treatment of B cell malignancies. To this date, application of CAR-T therapy beyond CD19 remains challenging due to the inability to control CAR-T reactivity in patients and the lack of tumor-associated antigens exclusively expressed by malignant cells. The interleukin-3 receptor alpha chain (CD123) is a promising immunotherapeutic target and associated with leukemia-initiating compartments in myeloid- or lymphoid derived diseases. However, in contrast to CD19, CD123 is a precarious target due to its prevalent expression on healthy hematopoietic stem and progenitor cells (HSPC) as well as endothelial cells. Thus, CAR-T lacking any fine-tuned control mechanisms are at risk to cause life threatening toxicities or can only act as bridging therapy to an allogeneic stem cell transplantation. To extend application of CAR-T therapy and safely redirect CAR-engineered T cells to challenging targets such as CD123, a switch-controllable universal CAR-T platform (UniCAR) was recently introduced. The UniCAR system consists of two components: (1) a non-reactive inducible second generation CAR with CD28/CD3ζ stimulation for an inert manipulation of T cells (UniCAR-T) and (2) soluble targeting modules (TM) enabling UniCAR-T reactivity in an antigen-specific manner. Here we provide late stage pre-clinical data for UniCAR-T in combination with a CD123-specific TM (TM123) for treatment of acute leukemia. Primary patient-derived CD123-positive leukemic blasts were efficiently eradicated by TM123-redirected clinical-grade manufactured UniCAR-T in vitro and in vivo. Activation, cytolytic responses and cytokine release were proven to be strictly switch-controlled. Moreover, anti-leukemic responses of UniCAR-T were demonstrated to be comparable to conventional CD123-specific CAR-T in vitro. In contrast to conventional CD123 CAR-T, TM123-redirected UniCAR-T discriminate between CD123high malignant cells and CD123low healthy cells with negligible toxicity towards HSPC in vivo. As 4-1BB mediated co-stimulation is known to enhance CAR-T activity in vivo, a novel CD123-specific targeting module bearing a covalently bound trimeric 4-1BB ligand (4-1BBL) was developed and characterized for co-stimulation at the leukemic site in trans. Specific binding of TM123-4-1BBL was demonstrated against native 4-1BB as well as CD123-positive leukemic blasts. In long-term tumor eradication models, TM123-4-1BBL ameliorated the killing capability of UniCAR-T in vitro. Additionally, the increased hydrodynamic radius of trimeric 4-1BBL-coupled TM123 prolonged plasma half-life and enhanced bioavailability in vivo. In conclusion, UniCAR-T maintain high anti-leukemic efficacy, while adding a sophisticated mechanism for immediate control to improve safety and versatility of CD123-directed CAR-T therapy. Moreover, switching between several TMs from short to moderate plasma half-life allows for an individualized treatment of various leukemic settings while minimizing potential adverse effects. Disclosures Loff: GEMoaB Monoclonals GmbH: Employment. Meyer:Cellex Patient Treatment GmbH: Employment. Dietrich:Cellex Patient Treatment GmbH: Employment. Spehr:Cellex Patient Treatment GmbH: Employment. Julia:Cellex Patient Treatment GmbH: Employment. Gründer:GEMoaB Monoclonals GmbH: Employment. Franke:GEMoaB Monoclonals GmbH: Employment. Bachmann:GEMoaB Monoclonals GmbH: Equity Ownership. Ehninger:Bayer: Research Funding; GEMoaB Monoclonals GmbH: Employment, Equity Ownership; Cellex Gesellschaft fuer Zellgewinnung mbH: Employment, Equity Ownership. Ehninger:GEMoaB Monoclonals GmbH: Employment, Equity Ownership; Cellex Gesellschaft fuer Zellgewinnung mbH: Equity Ownership. Cartellieri:Cellex Patient Treatment GmbH: Employment.

Published

2018

29. Targeting leukemia using an inducible universal chimeric antigen receptor (UniCAR) T cell technology

Author

Josephine Dietrich, M von Bonin, M. Hetzenecker, Julia Riewaldt, Simon Loff, G. Ehninger, Cordula Gründer, Johannes Spehr, Armin Ehninger, Marc Cartellieri, Jan-Erik Meyer, and Michael Bachmann

Subjects

Cancer Research, Transplantation, T cell, Immunology, Cell Biology, Biology, medicine.disease, Virology, Molecular biology, Chimeric antigen receptor, Leukemia, medicine.anatomical_structure, Oncology, medicine, Immunology and Allergy, Genetics (clinical)

Published

2017

30. Posttranscriptional regulation of c-Myc expression in adult murine HSCs during homeostasis and interferon-α-induced stress response

Author

Tobias Boch, Hannah Uckelmann, Marieke A.G. Essers, Armin Ehninger, Andreas Trumpp, Katja Müdder, and Barry P. Sleckman

Subjects

Immunology, Green Fluorescent Proteins, Endogeny, Mice, Transgenic, Biology, Biochemistry, Proto-Oncogene Proteins c-myc, Mice, Interferon, Stress, Physiological, medicine, Animals, Homeostasis, Progenitor cell, RNA Processing, Post-Transcriptional, Cells, Cultured, Progenitor, Messenger RNA, Reverse Transcriptase Polymerase Chain Reaction, Hematopoietic stem cell, Interferon-alpha, Cell Differentiation, Cell Biology, Hematology, Flow Cytometry, Hematopoietic Stem Cells, Fusion protein, Cell biology, Mice, Inbred C57BL, Haematopoiesis, medicine.anatomical_structure, Gene Expression Regulation, medicine.drug

Abstract

Previous studies have established pivotal roles for c-Myc and its homolog N-Myc in hematopoietic stem cell (HSC) maintenance and niche-dependent differentiation. However, it remains largely unclear how c-Myc expression is regulated in this context. Here, we show that HSCs and more committed progenitors express similar levels of c-myc transcripts. Using knock-in mice expressing a functional enhanced green fluorescent protein-c-Myc fusion protein under control of the endogenous c-myc locus, c-Myc protein levels were assessed. Although HSCs express low levels of c-Myc protein, its expression increases steadily during progenitor differentiation. Thus, mRNA and protein expression patterns differ significantly in stem/progenitor cells, suggesting that c-Myc expression is largely controlled posttranscriptionally. Moreover, interferon-α exposure, which activates dormant HSCs, strongly induces c-Myc expression at the protein level but not at the transcript level. This posttranscriptional mechanism of c-Myc regulation provides the blood system with a rapid way to adjust c-Myc expression according to demand during hematopoietic stress.

Published

2014

31. Redirection of CD4+ and CD8+ T lymphocytes via a novel antibody-based modular targeting system triggers efficient killing of PSCA+ prostate tumor cells

Author

Claudia, Arndt, Anja, Feldmann, Katrin, Töpfer, Stefanie, Koristka, Marc, Cartellieri, Achim, Temme, Armin, Ehninger, Gerhard, Ehninger, and Michael, Bachmann

Subjects

CD4-Positive T-Lymphocytes, Male, Mice, Antigens, Neoplasm, Cell Line, Tumor, Prostate, Animals, Humans, Prostatic Neoplasms, Immunotherapy, CD8-Positive T-Lymphocytes, GPI-Linked Proteins, Neoplasm Proteins

Abstract

There is still a need for new therapeutic options against prostate cancer. Conventional single-chain bispecific antibodies (bsAbs), that directly cross-link T cells and tumor cells, hold great potential for efficient tumor treatment. However, rapid development of novel bsAbs is hampered by laborious optimization to improve their efficacy and reduce potential side effects. To accelerate the development of a novel antibody tool for the redirection of T cells to different tumor-associated antigens, we recently introduced a modular targeting system.We here describe a novel modular system for treatment of prostate cancer by retargeting of T cells to the prostate stem cell antigen (PSCA). Functionality of the novel PSCA-specific modular system was investigated in vitro by T cell activation and chromium release assays as well as in immunodeficient mice.Similar to a conventional bsAb CD3-PSCA, the novel PSCA-specific modular system induces activation of both CD4+ and CD8+ T cells leading to secretion of pro-inflammatory cytokines and highly efficient target-specific tumor cell lysis. The novel TM was ready-to-use from the time point of construction and functional at low E:T ratios and picomolar concentrations without further optimization. In addition, the PSCA-specific modular system delays outgrowth of s.c. tumors in mice comparable to bsAb CD3-PSCA.We have developed a novel PSCA-specific modular system which triggers an efficient T cell-mediated killing of PSCA+ tumor cells in vitro and in vivo. The new Ab-based targeting strategy can functionally replace conventional bsAbs and allows a flexible redirection of T cells to different tumor-associated antigens.

Published

2014

32. Abstract B099: The UniCAR system: Inducible CAR T cells for precise reactivity and high efficacy against hematopoietic malignancies

Author

Malte von Bonin, Anja Feldmann, Simon Loff, Jan-Erik Meyer, Cordula Gründer, Armin Ehninger, Claudia Arndt, Johannes Spehr, Marc Cartellieri, Gerhard Ehninger, Josephine Dietrich, and Michael Bachmann

Subjects

Cancer Research, medicine.medical_treatment, T cell, Immunology, CD137, CD28, Immunotherapy, Biology, Chimeric antigen receptor, medicine.anatomical_structure, Antigen, Cancer research, medicine, Cytotoxic T cell, B cell

Abstract

During the past years promising clinical outcomes have been reported using immunotherapy for treatment of solid tumors and malignancies of the hematopoietic system. Since T cells act as key players in immune surveillance, an encouraging approach is to genetically engineer T cells with lenti- or retroviral vectors, in order to express artificial chimeric antigen receptors (CARs), directing them against cancer cells and leading to a distinct cytotoxic response. CARs are synthetic fusion proteins consisting of an antigen-binding moiety, commonly a tumor-associated antigen (TAA)-specific single-chain fragment variable (scFv), combined with activating signaling domains like the CD3-zeta chain. Signaling can be enhanced by adding co-stimulatory domains, such as the intracellular regions of CD28 or CD137. Although, CAR T cells showed promising results in patients with B cell malignancies, a major drawback of conventional CARs, bearing a tumor-antigen-binding moiety, is the uncontrollable continuous T cell activity. Hence, CAR T cells can achieve a sustained anti-tumoral response. However, reactivity against any healthy tissues expressing the target antigen might cause severe adverse effects. A chance to gain safety on CAR T cell approaches by retaining efficacy is offered through a novel universal binary CAR system (UniCAR). The system is based on a second generation CAR with an extracellular scFv binding domain, which is directed against a short non-immunogenic peptide motif instead of a cell surface antigen. Thus, engineered T cells are inert per se, remaining in a “sleeping mode” after re-infusion. Small protein links (targeting modules, TMs), consisting e.g. of TAA-specific scFvs harboring the small peptide epitope recognized by the UniCAR are used to redirect UniCAR expressing T cells in an antigen-specific manner. Primary results demonstrate that UniCAR driven T cell activation and cytotoxic effects against tumor cells are strictly dependent on the presence of the antigen-specific TMs. UniCAR T cells show high anti-tumor efficacy even at picomolar TM concentrations and low effector to target cell (e:t) ratios in vitro. After those proof-of-concept studies we disclose positive evidence of high efficacy UniCAR T cells with reactivity against CD123-positive acute myeloid leukemia (AML) and CD19-bearing acute lymphoblastic leukemia (ALL) cells. UniCAR T cell anti-tumor efficacy proofed to be superior when compared to conventional CAR T cells at low e:t ratios adjusted to the situation usually found in patients. Furthermore, UniCAR T cells pre-decorated with CD123-specific TMs in vitro are capable of prohibiting tumor engraftment of CD123-positive AML in vivo and persist in immunodeficient NSG mice. Ex vivo isolated UniCAR T cells retained cytotoxic potential against MOLM-13 cells for at least four month post transplantation fortifying the therapeutic potential in vitro and in vivo. The tremendous benefit of the novel UniCAR platform is the precise control of CAR T cell activity by regulating TM administration and dosage, preventing off side-toxicities arising from conventional CAR approaches. Moreover, the modular UniCAR system also enables combinatorial targeting strategies against several TAAs to increase therapy performance and circumvent the occurrence of tumor resistance mechanisms due to selectable compositions of target structures. Leukemia-related target antigens like CD19, CD20, CD22, CD33 or CD123 are conceivable therapy settings, offering advantages compared to monotherapeutic CAR-based therapies. Taken together, the modular composition of the UniCAR platform maintains the high anti-tumor potential of CAR-engrafted T cells, while introducing tight control mechanisms and unparalleled target flexibility. These features will allow a more sophisticated application of CAR technology and a reduction of adverse events in the clinical setting. Citation Format: Simon Loff, Malte v. Bonin, Josephine Dietrich, Jan-Erik Meyer, Anja Feldmann, Claudia Arndt, Johannes Spehr, Cordula Gründer, Gerhard Ehninger, Michael P. Bachmann, Armin Ehninger, Marc Cartellieri. The UniCAR system: Inducible CAR T cells for precise reactivity and high efficacy against hematopoietic malignancies [abstract]. In: Proceedings of the Second CRI-CIMT-EATI-AACR International Cancer Immunotherapy Conference: Translating Science into Survival; 2016 Sept 25-28; New York, NY. Philadelphia (PA): AACR; Cancer Immunol Res 2016;4(11 Suppl):Abstract nr B099.

Published

2016

33. Abstract 2313: Improved killing of tumor cells by a novel flexible antibody-based modular T cell retargeting system

Author

Anja Feldmann, Michael Bachmann, Armin Ehninger, Marc Cartellieri, Stefanie Koristka, Gerhard Ehninger, Claudia Arndt, Malte von Bonin, and Simon Loff

Subjects

0301 basic medicine, Cancer Research, Effector, Computer science, medicine.medical_treatment, T cell, Epitope, Chimeric antigen receptor, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, Oncology, Cancer immunotherapy, Antigen, Retargeting, Immunology, medicine, Cancer research, Cytotoxic T cell

Abstract

In recent years, bispecific antibodies (bsabs) and chimeric antigen receptors (CARs) emerged as promising candidates for an antigen-specific cancer immunotherapy. Bsabs and CARs redirect T cells in an antigen-specific manner towards tumor cells and unleash their enormous cytotoxic potential to attack the tumor. Nevertheless, several challenges have to be solved to pave the way for a more widespread application of both strategies. Both approaches are monotherapies bearing the inherent risk for development of antigen-loss tumor variants under treatment. In addition, due to their single antigen specificity each given bsab or CAR is only curative for a restricted number of tumor indications and long-lasting and demanding research is necessary to bring a new bsab- or CAR-based drug to patients in need. Moreover, current CAR T cell approaches do not allow for any control of the magnitude and duration of T cell reactivity, thus bearing the risk for overshooting anti-tumor reactions leading to severe side effects and ongoing destruction of healthy tissue carrying the target antigen after tumor clearance. To overcome these limitations, we recently introduced a novel flexible antibody-based modular platform (UniTARG) that can be rapidly and easily adapted for redirection of T cells to any TAA in both a bsAb- or CAR-setting. The UniTARG technology consists of a universal effector arm and individual targeting modules (TMs). The effector arm is either a universal CAR (UniCAR), which has specificity for a short peptide motif of 10 amino acids derived from a human nuclear protein, or a bsAb (UniMAB) with specificity for human CD3 on T cells and the respective peptide epitope. The antigen-specificity of the system is provided by TMs comprising a binding domain e.g., a tumor-antigen specific scFv, fused to the nuclear antigen motif recognized by the UniCAR/UniMAB binding domain. Here we provide first in vitro and in vivo prove of concept for these new approaches. Redirection of T cells armed with the universal effector modules was effective at picomolar concentrations of targeting modules directed against various antigens. The modular composition of both platforms prompted us to explore, if T cell retargeting against several antigens simultaneously might be feasible. Using either two single-specific TMs or single bi-specific TMs significantly enhanced specific lysis of tumor cells in vitro and durable responses in vivo were observed. Furthermore, our results proof that TMs against new targets can be developed in a couple of weeks and all TMs tested so far engaged effector module armed T cells with similar potencies. Taken together, the UniTARG platform technology represents a promising tool in the field of both bsAbs and CARs with the advantage of simultaneous or consecutive dual or even multispecific T cell retargeting. Furthermore the platform approach allows a rapid development of new therapeutic options against additional targets. Citation Format: Armin Ehninger, Marc Cartellieri, Anja Feldmann, Claudia Arndt, Stefanie Koristka, Simon Loff, Malte von Bonin, Gerhard Ehninger, Michael Bachmann. Improved killing of tumor cells by a novel flexible antibody-based modular T cell retargeting system. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr 2313.

Published

2016

34. Exploratory investigation of PSCA-protein expression in primary breast cancer and its clinical relevance

Author

Michael S. Kramer, Pauline Wimberger, Andreas Werner, Armin Ehninger, Friederike Kuithan, Barbara Richter, Katrin Friedrich, Jan Dominik Kuhlmann, Theresa Link, and Axel Gatzweiler

Subjects

Cancer Research, business.industry, Glycosylphosphatidylinositol, fungi, food and beverages, PSCA Protein, Prostate Stem Cell Antigen, carbohydrates (lipids), chemistry.chemical_compound, medicine.anatomical_structure, Oncology, chemistry, Prostate, Cancer research, Medicine, lipids (amino acids, peptides, and proteins), Clinical significance, Primary breast cancer, business, Surface protein

Abstract

e23267Background: Prostate stem cell antigen (PSCA) is a glycosylphosphatidylinositol (GPI)-anchored cell surface protein, which can be up-regulated in various human malignancies such as prostate, ...

Published

2016

35. C-Myc and its target FoxM1 are critical downstream effectors of constitutive androstane receptor (CAR) mediated direct liver hyperplasia

Author

David D. Moore, Mark J. Murphy, Armin Ehninger, Christelle Dubey, William Blanco-Bose, Wendong Huang, Andreas Trumpp, and Sandra Offner

Subjects

Pyridines, Receptors, Cytoplasmic and Nuclear, Mice, Transgenic, CDC20, Biology, Proto-Oncogene Proteins c-myc, Mice, Constitutive androstane receptor, Animals, Transcription factor, Constitutive Androstane Receptor, Cyclin, Cell Proliferation, Cyclin-dependent kinase 1, Hyperplasia, Hepatology, Forkhead Box Protein M1, Forkhead Transcription Factors, Cell cycle, Disease Models, Animal, Nuclear receptor, Liver, Cancer research, Hepatocytes, Signal transduction, Signal Transduction, Transcription Factors

Abstract

In the adult liver, 1,4-bis[2-(3,5-dichloropyridyloxy)] benzene (TCPOBOP), an agonist of the constitutive androstane receptor (CAR, NR1I3), produces rapid hepatomegaly in the absence of injury. In this study, we identify c-Myc as a gene induced by CAR and demonstrate that TCPOBOP-induced proliferation of hepatocytes depends on c-Myc function. Moreover, the TCPOBOP-induced cell cycle program (Cdc2, cyclins, MCM proteins, Cdc20, and genes implicated in the spindle assembly checkpoint) is severely impaired in c-Myc mutant livers. Strikingly, many of these genes overlap with a program controlled by the forkhead transcription factor FoxM1, known to control progression through S-phase and mitosis. Indeed, FoxM1 is also induced by TCPOBOP. Moreover, we show that c-Myc binds to the FoxM1 promoter in a TCPOBOP-dependent manner, suggesting a CAR -> c-Myc -> FoxM1 pathway downstream of TCPOBOP. Conclusion: Collectively, this study identifies c-Myc and FoxM1 mediated proliferative programs as key mediators of TCPOBOP-CAR induced direct liver hyperplasia.

Published

2008

36. Placental rescue reveals a sole requirement for c-Myc in embryonic erythroblast survival and hematopoietic stem cell function

Author

Christelle Adolphe, Rong Wang, Elisabeth J. Robertson, Armin Ehninger, Andreas Trumpp, and Nicole Dubois

Subjects

animal structures, Erythroblasts, Cell Survival, Placenta, Agm Region, Mice, Transgenic, Biology, survival, Gene, Models, Biological, Targeted Mutation, Proto-Oncogene Proteins c-myc, Mice, Mice Lacking, Erythroblast, Pregnancy, medicine, Morphogenesis, Animals, Progenitor cell, Molecular Biology, mouse, Alleles, Genetics, Transcriptional Control, Wild type, Hematopoietic stem cell, Embryo, Yolk-Sac Hematopoiesis, Hematopoietic Stem Cells, Intestinal Crypts, Embryonic stem cell, Immunohistochemistry, Cell biology, Haematopoiesis, c-Myc, medicine.anatomical_structure, Liver, Epiblast, Differentiation, Mouse Embryo, embryonic structures, hematopoietic stem cell, Female, embryonic hematopoiesis, fetal liver, Developmental Biology

Abstract

The c-Myc protein has been implicated in playing a pivotal role in regulating the expression of a large number of genes involved in many aspects of cellular function. Consistent with this view, embryos lacking the c-myc gene exhibit severe developmental defects and die before midgestation. Here, we show that Sox2Cre-mediated deletion of the conditional c-mycflox allele specifically in the epiblast (hence trophoectoderm and primitive endoderm structures are wild type) rescues the majority of developmental abnormalities previously characterized in c-myc knockout embryos, indicating that they are secondary defects and arise as a result of placental insufficiency. Epiblast-restricted c-Myc-null embryos appear morphologically normal and do not exhibit any obvious proliferation defects. Nonetheless, these embryos are severely anemic and die before E12. c-Myc-deficient embryos exhibit fetal liver hypoplasia,apoptosis of erythrocyte precursors and functionally defective definitive hematopoietic stem/progenitor cells. Specific deletion of c-mycflox in hemogenic or hepatocytic lineages validate the hematopoietic-specific requirement of c-Myc in the embryo proper and provide in vivo evidence to support a synergism between hematopoietic and liver development. Our results reveal for the first time that physiological levels of c-Myc are essential for cell survival and demonstrate that, in contrast to most other embryonic lineages, erythroblasts and hematopoietic stem/progenitor cells are particularly dependent on c-Myc function.

Published

2008

37. Abstract B021: Treatment with a novel targeting module, redirecting UniCAR T cells against PSCA, delays subcutaneous tumor growth and prolongs survival of tumor-bearing NSG mice

Author

Elham Pishali Bejestani, Marc Cartellieri, Michael Bachmann, Mechthild Krause, Malte von Bonin, Gerhard Ehninger, Michael H. Baumann, and Armin Ehninger

Subjects

Cancer Research, Adoptive cell transfer, Chemistry, medicine.medical_treatment, T cell, Immunology, Chimeric antigen receptor, Prostate Stem Cell Antigen, Immune system, Cell killing, medicine.anatomical_structure, Antigen, Cancer immunotherapy, Cancer research, medicine

Abstract

Background: The adoptive transfer of T cell engineered with chimeric antigen receptors (CARs) is currently considered a highly promising therapeutic option for treating so far incurable malignant diseases. In order to reduce adverse reactions associated with CAR engineered T cells, a flexible modular universal chimeric antigen receptor (UniCAR) platform is developed, which allows a precise control of CAR T cell reactivity to manage side effects while preserving efficacy. The UniCAR technology splits the signaling and antigen-binding aspects of conventional CARs into two individual components. The UniCAR is structurally similar to second-generation CARs, however the single chain variable fragment (scFv) does not recognize a cell surface antigen but a short peptide motif derived from a human nuclear autoantigen. Antigen-specificity and crosslinking of UniCAR expressing T cells to target cells is provided by a separate targeting module (TM) compromising a scFv, binding to specific cell surface antigens, fused to the aforementioned peptide motif. Thus, T cells engineered to express UniCARs remain inactivated after infusion, since the UniCAR target is not available for binding under physiological conditions. Only in the presence of the TM, antigen specific activation of UniCAR T cells occurs, which allows for a more sophisticated regulation. Methods: We developed a novel radio-immune target module (TM), which consists of an anti-PSCA (prostate stem cell antigen) scFv for redirecting of UniCARs to PSCA expressing tumor cells. Three different tags are fused in a row to the C-Terminus of the scFv to functionalize the molecule for combined immune- and radiotherapy. First, a ten amino acid (aa) long tag mediates the crosslink to T cells genetically modified with the UniCAR. Further downstream, a peptide tag (Rx) for enhanced conjugation of radionuclides and finally, a 6xhistidine (His) tag are located. TM-Rx efficacy was evaluated for target cell killing in-vitro and compared to a TM without Rx-tag. In-vivo efficacy of the TM-Rx was also investigated in a high and low-tumor burden mouse model. Results: Rx-TM and TM equivalently kill PSCA-expressing tumor cells in-vitro in presence of UniCARs in an E:T (Effector:Target) ratio of 1:1 after 24 hours. UniCAR T cell engrafted NSG (NOD.Cg-Prkdcscid Il2rgtm1Wjl/SzJ) mice show no clinical signs of autoimmunity neither in presence nor absence of the TM. One week treatment with TM delays subcutaneous tumor growth and prolongs survival of tumor bearing, UniCAR T cell engrafted NSG mice. Longterm infiltration of tumor tissue by UniCARs could be observed over 16 weeks in the high and low-tumor burden ectopic carcinoma model. Conclusion: The UniCAR technology shows efficacy both in-vitro and in-vivo. Extension of the TM with an additional tag does not impair functionality of the UniCAR platform. Short-treatment prolongs survival of tumor bearing mice but does not lead to cure, therefore combination with other treatment modalities e.g. radiation oncology seems reasonable. Citation Format: Elham Pishali Bejestani, Malte von Bonin, Marc Cartellieri, Armin Ehninger, Mechthild Krause, Michael Baumann, Gerhard Ehninger, Michael Bachmann. Treatment with a novel targeting module, redirecting UniCAR T cells against PSCA, delays subcutaneous tumor growth and prolongs survival of tumor-bearing NSG mice. [abstract]. In: Proceedings of the CRI-CIMT-EATI-AACR Inaugural International Cancer Immunotherapy Conference: Translating Science into Survival; September 16-19, 2015; New York, NY. Philadelphia (PA): AACR; Cancer Immunol Res 2016;4(1 Suppl):Abstract nr B021.

Published

2016

38. Emerging role of SUMO in pancreatic beta-cells

Author

H Mziaut, Michele Solimena, and Armin Ehninger

Subjects

medicine.medical_specialty, SUMO-1 Protein, Maf Transcription Factors, Large, Protein Conformation, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, SUMO protein, Saccharomyces cerevisiae, Biology, Biochemistry, DNA-binding protein, Models, Biological, Endocrinology, Internal medicine, Insulin-Secreting Cells, Gene expression, medicine, Transcriptional regulation, Humans, Insulin, Genetic Predisposition to Disease, Receptor-Like Protein Tyrosine Phosphatases, Class 8, Regulation of gene expression, Homeodomain Proteins, fungi, Biochemistry (medical), food and beverages, General Medicine, DNA-Binding Proteins, Protein Transport, Diabetes Mellitus, Type 1, Gene Expression Regulation, Trans-Activators, Signal transduction, Protein Processing, Post-Translational, Protein Binding, Signal Transduction

Abstract

Post-translational attachment of small ubiquitin-like modifier (SUMO), defined as SUMOylation, can affect the localization, interactions, stability and/or activity of substrate proteins, and thus can participate in a large variety of cellular processes. Most SUMO substrates are involved in transcriptional regulation. Hence, SUMOylation can either activate or, more commonly, repress gene transcription. The modulation of gene expression by SUMO through diverse mechanisms and specifically the recent findings concerning SUMOylation in pancreatic beta-cells are reviewed.

Published

2007

39. Improved Killing of AML Blasts By Dual-Targeting of CD123 and CD33 Via Unitarg a Novel Antibody-Based Modular T Cell Retargeting System

Author

Anja Feldmann, Gerhard Ehninger, Martin Bornhäuser, Marc Cartellieri, Michael Bachmann, Claudia Arndt, Stefanie Koristka, Armin Ehninger, and Malte von Bonin

Subjects

Chemistry, Effector, T cell, medicine.medical_treatment, Immunology, Cell Biology, Hematology, Biochemistry, Epitope, Chimeric antigen receptor, medicine.anatomical_structure, Tumor Escape, Antigen, Cancer immunotherapy, Cancer cell, Cancer research, medicine

Abstract

Acute myeloid leukemia (AML) is a hematologic malignancy of the myeloid line with high prevalence in older patients. As complete eradication of metastatic cancer cells is often not achieved by standard therapies, alternative treatment modalities are urgently needed. In recent years, bispecific antibodies (bsAbs) and chimeric antigen receptors (CARs) emerged as promising candidates for an antigen-specific cancer immunotherapy. Both bsAbs and CARs are able to redirect T cells for efficient tumor cell lysis. Nevertheless, the development of a novel TAA specific bsAb or a CAR is a long lasting process. Therefore, we recently introduced a novel antibody-based modular platform (UniTARG) that can be rapidly and easily adapted for redirection of T cells to any TAA in both a bsAb or CAR related manner. The modular UniTARG system distributes the effector arm (the anti-CD3 domain or CAR) and the anti-TAA binding domain to two separate molecules: (I) an exchangeable target module (TM) comprising an anti-TAA binding moiety and a short peptide epitope (E5B9), and (II) a universal effector unit. The effector systems represent either a bsAb with specificity for CD3 and a peptide epitope (E5B9) termed UniMAB or a CAR directed to the E5B9 epitope (UniCAR). Thus, TMs can form a complex with the respective effector system that facilitates the cross-linkage of tumor and T cells similar to conventional bsAbs or CARs. For redirection of T cells to any kind of TAA only the binding moiety of the TM has to be adapted what saves costs and time. To increase tumor specificity and to reduce the risk of tumor escape variants, the modular UniTARG system further offers the possibility to apply simultaneously different monospecific or even bispecific TMs recognizing two TAAs. For proof of concept of a dual targeting using the UniTARG system we selected as TAA on AML blasts the molecules CD33 and CD123. They represent promising target antigens as they are overexpressed on both rapidly proliferating terminal AML blasts and leukemic stem cells which might be responsible for disease relapse after initial chemotherapy. Thus, we generated an anti-CD123 TM and anti-CD33 TM that can be applied within the modular system for single-targeting or that can be combined for dual-targeting of AML blasts. By fusion of the anti-CD123 and anti-CD33 domains via the E5B9 epitope a bispecific TM was further constructed. As revealed by cytotoxicity assays with CD33+ CD123+ AML cell lines, the novel mono- and bispecific TMs can be easily applied to the modular systems to trigger highly potent tumor cell lysis at low E:T ratios and picomolar Ab concentrations. By using the dual-targeting approach we can show that lysis of CD123+ CD33+ AML blasts can be considerably improved in comparison to the mono-specific strategy. Overall, due to the ease and cost-effectiveness of development the UniTARG platform technology represents a promising tool in the field of both bsAbs and CARs with the advantage of simultaneous or consecutive dual or even multispecific targeting. This approach might additionally improve anti-tumor activity by increasing tumor specificity and diminishing off-target effects. Disclosures Cartellieri: Cellex Patient Treatment GmbH: Employment. Ehninger:GEMoaB Monoclonals GmbH: Employment, Patents & Royalties: related to the UniTARG system. Ehninger:GEMoaB Monoclonals GmbH: Equity Ownership, Patents & Royalties: related to the UniTARG system. Bachmann:GEMoaB Monoclonals GmbH: Equity Ownership, Patents & Royalties: related to the UniTARG system.

Published

2015

40. Unicar: A Novel Modular Retargeting Platform Technology for CAR T Cells

Author

Anja Feldmann, Simon Loff, Claudia Arndt, Elham Pishali Bejestani, Michael Bachmann, Marc Cartellieri, Gerhard Ehninger, Stefanie Koristka, Malte von Bonin, and Armin Ehninger

Subjects

Adoptive cell transfer, biology, Chemistry, T cell, Immunology, T-cell receptor, CD28, Cell Biology, Hematology, Biochemistry, Epitope, Chimeric antigen receptor, CD19, Cell biology, medicine.anatomical_structure, Antigen, medicine, biology.protein

Abstract

The adoptive transfer of T cells engineered with chimeric antigen receptors (CARs) is currently considered as a highly promising therapeutic option for treatment of otherwise incurable malignant diseases. CARs combine the cellular and humoral arm of the immune response by assembling a single-chain fragment variable (scFv) as binding moiety which provides the antigen-specificity and an activating immune receptor. It has been demonstrated both in vitro and in vivo, that CAR engrafted effector T cells mediate long-lasting anti-tumor responses. Despite encouraging clinical efficacy targeting CD19 in recent clinical trials, the appearance of potentially life-threatening adverse reactions and the lack of control mechanisms once initiated, prevent more widespread application of the CAR technology. To overcome limitations of conventional CAR T cells, a unique chimeric antigen receptor (UniCAR) technology was developed (Fig. 1) which allows precise control of CAR T cell reactivity, thus lowering the risk of side effects while preserving efficacy. Moreover, the UniCAR technology enables the retargeting of engrafted T cells against more than one antigen simultaneously or subsequently, thus reducing the risk for development of antigen-loss tumor variants under treatment. The UniCAR technology splits the signaling and antigen-binding aspects of conventional CAR into two individual components. T cells are engineered to express a universal CAR (UniCAR), which has specificity for a short peptide motif of 10 amino acids derived from a human nuclear protein. Thus, T cells engineered to express UniCAR remain inactivated after re-infusion, since the UniCAR target is not available for binding under physiological conditions. The ultimate antigen-specificity of the system is provided separately by targeting modules (TMs) comprising a binding domain e.g., a tumor-antigen specific scFv, fused to the nuclear antigen motif recognized by the UniCAR binding domain. Here we provide first in vitro and in vivo prove of concept for this new approach. Antigen-specific redirection of T cells armed with the universal CAR in the presence of different targeting modules against various antigens (CD33, CD123, CD19, CD20, PSCA, PSMA,) was effective at femtomolar concentrations of the targeting module both. Taken together, the modular nature of UniCAR technology will allow retargeting of autologous, patient-derived T cells to several antigens under controlled pharmacological conditions and has the potential to become a highly effective treatment option for late stage cancer patients with reduced risks for side effects. Figure 1. Schematic representation of T cell recruitment with the modular UniCAR system. The UniCAR T cell recruitment system consists of two separated units. The first unit is the UniCAR expressed on T cells with a single-chain fragment variable (scFv) specific for a short 10 aa long peptide motif. The intracellular signalling domain of the UniCAR contains a costimulatory domain derived from CD28 and the T cell receptor z chain. The second unit is a targeting molecule (TM) which consists of a scFv fused to the peptide epitope. The cross-linkage of T cell and target cell is mediated by interaction between the UniCAR binding domain on T cells and target cell binding TM. Figure 1. Schematic representation of T cell recruitment with the modular UniCAR system. / The UniCAR T cell recruitment system consists of two separated units. The first unit is the UniCAR expressed on T cells with a single-chain fragment variable (scFv) specific for a short 10 aa long peptide motif. The intracellular signalling domain of the UniCAR contains a costimulatory domain derived from CD28 and the T cell receptor z chain. The second unit is a targeting molecule (TM) which consists of a scFv fused to the peptide epitope. The cross-linkage of T cell and target cell is mediated by interaction between the UniCAR binding domain on T cells and target cell binding TM. Disclosures Cartellieri: Cellex Patient Treatment GmbH: Employment. Loff:GEMoaB Monoclonals GmbH: Employment. Ehninger:GEMoaB Monoclonals GmbH: Employment, Patents & Royalties: related to the UniTARG system. Ehninger:GEMoaB Monoclonals GmbH: Equity Ownership; Cellex Patient Treatment GmbH: Equity Ownership. Bachmann:GEMoaB Monoclonals GmbH: Equity Ownership, Patents & Royalties: related to the UniTARG system.

Published

2015

41. Synergy of glucose and growth hormone signalling in islet cells through ICA512 and STAT5

Author

Michele Solimena, Anke Altkrüger, Hassan Mziaut, Mirko Trajkovski, Myung-Shik Lee, Darja Schmidt, Armin Ehninger, Regis P. Lemaitre, Stephan Kersting, Hans-Detlev Saeger, David N. Drechsel, and Stefan Müller

Subjects

Transcription, Genetic, medicine.medical_treatment, SUMO protein, Protein tyrosine phosphatase, Autoantigens, Exocytosis, Islets of Langerhans, Mice, medicine, STAT5 Transcription Factor, Animals, Receptor-Like Protein Tyrosine Phosphatases, Class 8, ddc:610, Tyrosine, Phosphorylation, STAT5, Cells, Cultured, Cell Nucleus, Mice, Knockout, biology, Insulin, Secretory Vesicles, Membrane Proteins, Cell Biology, Protein Inhibitors of Activated STAT, Cell biology, Mice, Inbred C57BL, Insulin receptor, Glucose, Biochemistry, Growth Hormone, biology.protein, Small Ubiquitin-Related Modifier Proteins, Protein Tyrosine Phosphatases, Protein Binding, Signal Transduction

Abstract

Nutrients and growth hormones promote insulin production and the proliferation of pancreatic beta-cells. An imbalance between ever-increasing metabolic demands and insulin output causes diabetes. Recent evidence indicates that beta-cells enhance insulin gene expression depending on their secretory activity. This signalling pathway involves a catalytically inactive receptor tyrosine phosphatase, ICA512, whose cytoplasmic tail is cleaved on glucose-stimulated exocytosis of insulin secretory granules and then moves into the nucleus, where it upregulates insulin transcription. Here, we show that the cleaved cytosolic fragment of ICA512 enhances the transcription of secretory granule genes (including its own gene) by binding to tyrosine phosphorylated signal transducers and activators of transcription (STAT) 5 and preventing its dephosphorylation. Sumoylation of ICA512 by the E3 SUMO ligase PIASy, in turn, may reverse this process by decreasing the binding of ICA512 to STAT5. These findings illustrate how the exocytosis of secretory granules, through a retrograde pathway that sustains STAT activity, converges with growth hormone signalling to induce adaptive changes in beta-cells in response to metabolic demands.

Published

2005

42. Development of a Bispecific Antibody-Releasing Stem Cell System for the Eradication of Acute Myeloid Leukemia Blasts Via Redirected Immune Effector Cells

Author

Gerhard Ehninger, Claudia Arndt, Anja Feldmann, Irene Michalk, Michael Bachmann, Martin Bornhäuser, Roberta Aliperta, Stefanie Koristka, Marc Cartellieri, and Armin Ehninger

Subjects

business.industry, T cell, Immunology, Mesenchymal stem cell, Cell Biology, Hematology, Biochemistry, Minimal residual disease, Cell killing, medicine.anatomical_structure, Antigen, Cancer cell, medicine, Stem cell, business, CD8

Abstract

Despite many years of research and great advances in the field, acute myeloid leukemia (AML) still remains one of the most challenging battle fields in the context of hematologic malignancies treatment. Although AML patients initially respond to conventional chemotherapy, a complete remission is rarely achieved and 5-year survival rates remain low especially in elderly patients. Hence, there is a pressing need for novel effective strategies for AML treatment to prevent relapse and treat minimal residual disease (MRD). The use of recombinant bispecific antibodies (bsAbs) for retargeting effector T lymphocytes towards cancer cells is recently emerging as a promising immunotherapeutic approach for tumor treatment. This class of small molecules is designed to bind simultaneously to a pre-defined tumor-associated antigen (TAA) on tumor cells and the activating CD3 complex on T cells. The cross-linkage of immune effector cell and tumor cell leads to a tumor-specific T cell activation and efficient target cell killing independently of the T cell receptor specificity. However, due to their low molecular mass, bsAbs have a short life span in vivo and consequently have to be continuously administrated to patients over prolonged time spans of several weeks to achieve clinical responses. As an alternative to continuous exogenous infusions of short-lived Abs we examined the use of engineered bone marrow-derived human mesenchymal stem cells (hMSCs) as cellular vehicles for the constant production and secretion of a fully humanized anti-CD33-anti-CD3 bsAb that targets the surface molecule CD33, which is widely overexpressed on AML blasts. Our studies demonstrate that gene-modified hMSCs are effective in releasing the bsAb at sufficient amounts to activate and redirect both human primary CD4+ and CD8+T cells from healthy donors against AML cells expressing varying levels of the CD33 antigen, leading to an efficient T cell-mediated tumor cell killing at low effector to target cell ratios and Ab concentrations. Most importantly, we could demonstrate that patient-derived T cells were able to suppress autologous AML blasts upon Ab-mediated cross-linkage over prolonged period of time without being affected by the presence of the modified hMSCs. Additional improvement of this system was achieved by the artificial expression of T cell co-stimulatory 4-1BB ligand (CD137L) on the hMSCs surface. The additional co-stimulatory signal provided by the engineered hMSCs resulted in an enhanced T cell proliferation, a higher pro-inflammatory cytokine release, and consequently in a more pronounced specific tumor cell killing already at earlier time-points. Taken together, our data could demonstrate that continuous in situ delivery of the anti-CD33-anti-CD3 bsAb by genetically modified hMSCs facilitates efficient activation of T cells for specific and efficient killing of AML blasts over prolonged period of time. Furthermore, as promising perspective of this approach for future in vivo application we are currently investigating on the development of biocompatible synthetic scaffolds as transplantable biomaterial-based production platforms for genetically engineered hMSCs as locally confined vehicle of immunotherapeutics. The implantation of these small engineered devices would ensure that the delivery of the anti-cancer agents can be controlled and stopped after tumor clearance by removing the scaffold at a desired time point. In this way, administration of ex vivo gene-modified hMSCs embedded in appropriate scaffolds would result in a continuous in situ production of recombinant Abs for effective and persistent levels of these therapeutic agents over time with low risk of side effects. Disclosures Cartellieri: Cellex Patient Treatment GmbH, Dresden, Germany: Employment. Ehninger:GEMoaB Monoclonals GmbH, Dresden, Germany: Employment, Patents & Royalties. Ehninger:GEMoaB Monoclonals GmbH, Dresden, Germany: Consultancy, Patents & Royalties. Bachmann:GEMoaB Monoclonals GmbH, Dresden, Germany: Consultancy, Patents & Royalties.

Published

2014

43. Flexible Antigen-Specific Redirection of Human Regulatory T Cells Via a Novel Universal Chimeric Antigen Receptor System

Author

Michael Bachmann, Claudia Arndt, Gerhard Ehninger, Roberta Aliperta, Malte von Bonin, Armin Ehninger, Stefanie Koristka, Martin Bornhäuser, Simon Loff, Irene Michalk, Anja Feldmann, and Marc Cartellieri

Subjects

Adoptive cell transfer, education.field_of_study, Immunology, Population, FOXP3, chemical and pharmacologic phenomena, Cell Biology, Hematology, Biology, Biochemistry, Chimeric antigen receptor, Epitope, Immune system, Antigen, IL-2 receptor, education

Abstract

Based on compelling evidence from a vast number of in vitro and in vivostudies, Tregs have become an attractive cell population to treat or even prevent auto- and alloimmunity including Graft-versus-Host disease (GvHD). However, several safety concerns still exist as for example the risk of global immunosuppression using polyclonal Tregs. In fact, experiments in mice showed that adoptive transfer or induction of antigen-specific Tregs is more potent regarding suppression of pathogenic immune responses when compared to polyclonal Treg populations. Unfortunately, the isolation and expansion of naturally occurring antigen-specific Tregs is technically difficult, labour-intensive, and time-consuming. An attractive way to overcome these limitations and to endow polyclonal Treg populations with a desired antigen-specificity is their engraftment with chimeric antigen receptors (CARs). In this context, CAR-modification represents a promising approach to redirect polyclonal Tregs in an antigen-specific manner to suppress ongoing self-destructive immune responses at the site of inflammation. Nevertheless, until now redirection of CAR-engineered T cells is limited to a single target antigen, restricting this approach to an unflexible monospecific therapy. Therefore, we developed a more flexible universal CAR (UCAR) platform that allows redirection of T cells to an in principal unrestricted number of surface antigens. T cells are engrafted with UCARs that bind to a small peptide epitope derived from a human nuclear protein. Cross-linkage to target cells is mediated by independent target modules that provide antigen-specificity and comprise the peptide epitope recognized by the UCAR. In order to target different tissue antigens, the target modules can easily be exchanged. Thereby, once established, the treatment strategy can easily be applied to various auto- and alloimmune diseases. At present, the CD45RA+ population is the Treg subset of choice for a clinical application as these cells have the highest capacity to maintain phenotypic and functional Treg properties upon prolonged ex vivo expansion. Here we show that highly pure, sorted CD4+CD25+CD127lowCD45RA+ Tregs can be genetically manipulated using lentiviral gene transfer, resulting in approximately 70 % of UCAR-expressing Treg cells. The transduction procedure itself did not affect the phenotype of UCAR-engineered Tregs as it was similar to non-transduced wildtype cells. Both Treg populations presevered FOXP3 expression even after prolonged in vitro cultivation (> 95 % FOXP3+). Upon incubation with antigen-positive target cells and a respective target module UCAR-engineered Tregs upregulate the activation markers CD69 and LAP demonstrating that the cells can be restimulated antigen-specifically. Most importantly, UCAR-engrafted Tregs were functionally activated upon antigen encounter, demonstrated by suppression of proliferation and expansion of cocultured autologous T effector cells. Taken together, our results pave the way towards an application of UCAR technology for a site-specific recruitment of CAR-modified Tregs into inflamed tissues aiming at re-establishing immune homeostasis. Due to its high flexibility UCAR-engrafted Tregs can easily and universally be used for treatment of various autoimmune diseases or GvHD just by exchanging the tissue-specific target modules. Disclosures Cartellieri: Cellex Patient Treatment GmbH: Employment. Ehninger:GEMoaB GmbH: Employment, Patents & Royalties. Ehninger:GEMoaB GmbH: Consultancy, Patents & Royalties. Bachmann:GEMoaB GmbH: Consultancy, Patents & Royalties.

Published

2014

44. Distribution and levels of cell surface expression of CD33 and CD123 in acute myeloid leukemia

Author

Armin Ehninger, Martin Wermke, M von Bonin, Christoph Röllig, G. Ehninger, Michael Kramer, Christian Thiede, Martin Bornhäuser, Uta Oelschlägel, Anja Feldmann, and Michael Bachmann

Subjects

Adult, Male, NPM1, Myeloid, Adolescent, Gemtuzumab ozogamicin, Sialic Acid Binding Ig-like Lectin 3, CD33, Interleukin-3 Receptor alpha Subunit, Biology, Young Adult, Risk Factors, Immunotoxin, hemic and lymphatic diseases, medicine, Humans, Aged, Aged, 80 and over, Myeloid leukemia, Hematology, Middle Aged, Flow Cytometry, medicine.disease, Leukemia, Myeloid, Acute, Leukemia, medicine.anatomical_structure, fms-Like Tyrosine Kinase 3, Oncology, Fms-Like Tyrosine Kinase 3, Immunology, Cancer research, Female, Original Article, Nucleophosmin, medicine.drug

Abstract

Owing to the more recent positive results with the anti-CD33 immunotoxin gemtuzumab ozogamicin, therapy against acute myeloid leukemias (AMLs) targeting CD33 holds many promises. Here, CD33 and CD123 expression on AML blasts was studied by flow cytometry in a cohort of 319 patients with detailed information on French–American–British/World Health Organization (FAB/WHO) classification, cytogenetics and molecular aberrations. AMLs of 87.8% express CD33 and would therefore be targetable with anti-CD33 therapies. Additionally, 9.4% of AMLs express CD123 without concomitant CD33 expression. Thus, nearly all AMLs could be either targeted via CD33 or CD123. Simultaneous presence of both antigens was observed in 69.5% of patients. Most importantly, even AMLs with adverse cytogenetics express CD33 and CD123 levels comparable to those with favorable and intermediate subtypes. Some patient groups with unfavorable alterations, such as FMS-related tyrosine kinase 3-internal tandem duplication (FLT3-ITD) mutations, high FLT3-ITD mutant/wild-type ratios and monosomy 5 are even characterized by high expression of CD33 and CD123. In addition, blasts of patients with mutant nucleophosmin (NPM1) revealed significantly higher CD33 and CD123 expression pointing toward the possibility of minimal residual disease-guided interventions in mutated NPM1-positive AMLs. These results stimulate the development of novel concepts to redirect immune effector cells toward CD33- and CD123-expressing blasts using bi-specific antibodies or engineered T cells expressing chimeric antigen receptors.

Published

2014

45. Loss of sparc protects hematopoietic stem cells from the toxic effects of repeated cycles of chemotherapy by accelerating their return to quiescence

Author

Armin Ehninger, Andreas Trumpp, and Tobias Boch

Subjects

Cancer Research, Chemotherapy, genetic structures, business.industry, medicine.medical_treatment, Cancer, Cell Biology, Hematology, medicine.disease, eye diseases, Haematopoiesis, Genetics, medicine, Cancer research, sense organs, Stem cell, business, Molecular Biology

Abstract

P1068 LOSS OF SPARC PROTECTS HEMATOPOIETIC STEM CELLS FROM THE TOXIC EFFECTS OF REPEATED CYCLES OF CHEMOTHERAPY BY ACCELERATING THEIR RETURN TO QUIESCENCE Armin Ehninger, Tobias Boch, and Andreas Trumpp Division of Stem Cells and Cancer, German Cancer Research Center (DKFZ), Heidelberg, Germany; Heidelberg Institute for Stem Cell Technology and Experimental Medicine (HI-STEM), Heidelberg, Germany

Published

2013

46. Hematopoietic Stem Cell Function and Survival Depend on c-Myc and N-Myc Activity

Author

Barbara Varnum-Finney, Irwin D. Bernstein, Anne Wilson, H. Robson MacDonald, Armin Ehninger, Elisa Laurenti, Pei Feng Cheng, William Blanco-Bose, Isabel Ferrero, Robert N. Eisenman, Paul S. Knoepfler, and Andreas Trumpp

Subjects

Pancytopenia, Proliferation, Expression, Gene, Granzymes, Self-Renewal, Mice, 0302 clinical medicine, Granzyme-B, Cells, Cultured, Mice, Knockout, 0303 health sciences, Graft Survival, Hematopoietic Stem Cell Transplantation, Hematopoietic stem cell, Progenitor Cells, Cell Differentiation, 3. Good health, Endothelial stem cell, Haematopoiesis, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Differentiation, Serine-Protease Inhibitor-6, Molecular Medicine, Stem cell, Signal Transduction, Animals, Cell Differentiation/genetics, Cell Lineage/genetics, Cell Proliferation, Cell Survival/genetics, Graft Survival/genetics, Granzymes/metabolism, Hematopoiesis/physiology, Hematopoietic Stem Cell Transplantation/methods, Hematopoietic Stem Cells/cytology, Hematopoietic Stem Cells/metabolism, Pancytopenia/genetics, Pancytopenia/physiopathology, Proto-Oncogene Proteins c-myc/genetics, Signal Transduction/genetics, Stress, Physiological/genetics, Cell Survival, Activation, Biology, Proto-Oncogene Proteins c-myc, 03 medical and health sciences, Stress, Physiological, Genetics, medicine, Cell Lineage, Family, Progenitor cell, 030304 developmental biology, Innate immune system, Cell Biology, Hematopoietic Stem Cells, STEMCELL, Hematopoiesis, Apoptosis, Cancer research, Bone marrow

Abstract

SummaryMyc activity is emerging as a key element in acquisition and maintenance of stem cell properties. We have previously shown that c-Myc deficiency results in accumulation of defective hematopoietic stem cells (HSCs) due to niche-dependent differentiation defects. Here we report that immature HSCs coexpress c-myc and N-myc mRNA at similar levels. Although conditional deletion of N-myc in the bone marrow does not affect hematopoiesis, combined deficiency of c-Myc and N-Myc (dKO) results in pancytopenia and rapid lethality. Interestingly, proliferation of HSCs depends on both myc genes during homeostasis, but is c-Myc/N-Myc independent during bone marrow repair after injury. Strikingly, while most dKO hematopoietic cells undergo apoptosis, only self-renewing HSCs accumulate the cytotoxic molecule GranzymeB, normally employed by the innate immune system, thereby revealing an unexpected mechanism of stem cell apoptosis. Collectively, Myc activity (c-Myc and N-Myc) controls crucial aspects of HSC function including proliferation, differentiation, and survival.