Your search keyword '"UniCAR"' showing total 28 results

1. FLT3‐directed UniCAR T‐cell therapy of acute myeloid leukaemia.

Author

Peschke, J. C., Bergmann, R., Mehnert, M., Gonzalez Soto, K. E., Loureiro, L. R., Mitwasi, N., Kegler, A., Altmann, H., Wobus, M., Máthé, D., Szigeti, K., Feldmann, A., Bornhäuser, M., Bachmann, M., Fasslrinner, F., and Arndt, C.

Subjects

*ACUTE myeloid leukemia, *T cells, *CHIMERIC antigen receptors, *PROTEIN-tyrosine kinases

Abstract

Summary: Adaptor chimeric antigen receptor (CAR) T‐cell therapy offers solutions for improved safety and antigen escape, which represent main obstacles for the clinical translation of CAR T‐cell therapy in myeloid malignancies. The adaptor CAR T‐cell platform 'UniCAR' is currently under early clinical investigation. Recently, the first proof of concept of a well‐tolerated, rapidly switchable, CD123‐directed UniCAR T‐cell product treating patients with acute myeloid leukaemia (AML) was reported. Relapsed and refractory AML is prone to high plasticity under therapy pressure targeting one single tumour antigen. Thus, targeting of multiple tumour antigens seems to be required to achieve durable anti‐tumour responses, underlining the need to further design alternative AML‐specific target modules (TM) for the UniCAR platform. We here present the preclinical development of a novel FMS‐like tyrosine kinase 3 (FLT3)‐directed UniCAR T‐cell therapy, which is highly effective for in vitro killing of both AML cell lines and primary AML samples. Furthermore, we show in vivo functionality in a murine xenograft model. PET analyses further demonstrate a short serum half‐life of FLT3 TMs, which will enable a rapid on/off switch of UniCAR T cells. Overall, the presented preclinical data encourage the further development and clinical translation of FLT3‐specific UniCAR T cells for the therapy of AML. [ABSTRACT FROM AUTHOR]

Published

2023

2. Multivalent adaptor proteins specifically target NK cells carrying a universal chimeric antigen receptor to ErbB2 (HER2)-expressing cancers.

Author

Pfeifer Serrahima, Jordi, Zhang, Congcong, Oberoi, Pranav, Bodden, Malena, Röder, Jasmin, Arndt, Claudia, Feldmann, Anja, Kiefer, Anne, Prüfer, Maren, Kühnel, Ines, Tonn, Torsten, Bachmann, Michael, and Wels, Winfried S.

Subjects

*KILLER cells, *CHIMERIC antigen receptors, *ADAPTOR proteins, *CELL surface antigens, *CHIMERIC proteins, *PROTEIN engineering, *T cell receptors

Abstract

Chimeric antigen receptor (CAR)-engineered immune effector cells constitute a promising approach for adoptive cancer immunotherapy. Nevertheless, on-target/off-tumor toxicity and immune escape due to antigen loss represent considerable challenges. These may be overcome by adaptor CARs that are selectively triggered by bispecific molecules that crosslink the CAR with a tumor-associated surface antigen. Here, we generated NK cells carrying a first- or second-generation universal CAR (UniCAR) and redirected them to tumor cells with so-called target modules (TMs) which harbor an ErbB2 (HER2)-specific antibody domain for target cell binding and the E5B9 peptide recognized by the UniCAR. To investigate differential effects of the protein design on activity, we developed homodimeric TMs with one, two or three E5B9 peptides per monomer, and binding domains either directly linked or separated by an IgG4 Fc domain. The adaptor molecules were expressed as secreted proteins in Expi293F cells, purified from culture supernatants and their bispecific binding to UniCAR and ErbB2 was confirmed by flow cytometry. In cell killing experiments, all tested TMs redirected NK cell cytotoxicity selectively to ErbB2-positive tumor cells. Nevertheless, we found considerable differences in the extent of specific cell killing depending on TM design and CAR composition, with adaptor proteins carrying two or three E5B9 epitopes being more effective when combined with NK cells expressing the first-generation UniCAR, while the second-generation UniCAR was more active in the presence of TMs with one E5B9 sequence. These results may have important implications for the further development of optimized UniCAR and target module combinations for cancer immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2023

3. 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

4. Calidad de vida de pacientes pediátricos posterior a cirugía de cierre de comunicación interventricular en la Unidad de Cirugía Cardiovascular (UNICAR) de Guatemala 2014-2017

Author

Sergio Andrés Quiroa Valdez and Mauricio O'connell

Subjects

enfermedad cardiaca congénita, comunicación interventricular, calidad de vida, PedsQL, sobrevida, UNICAR, Medicine (General), R5-920

Abstract

Introducción: En los últimos años se ha observado un aumento en el diagnóstico de anomalías cardíacas congénitas dado las mejoras en cuidados prenatales y métodos de imagen de alta tecnología. En Guatemala, exsite una alta incidencia de cardiopatías cardíacas congénitas pero no hay un estudio que busque determinar los cambios en la calidad de vida que estos pacientes experimentan luego de la corrección quirúrgica. Objetivo: El propósito de este estudio fue determinar la calidad de vida en pacientes pediátricos, con diagnóstico de comunicación interventricular (CIV) posterior a cirugía en UNICAR en los años 2014-2017. Metodología: Se hizo una revisión de expendientes y se aplicó la encuesta Pediatrics Quality of life inventory 4.0 (PedsQL 4.0)11 por vía telefónica a los pacientes seleccionados. Resultados: De los 30 expedientes revisados, 23 (77%) participaron, 9 (39%) hombres y 14 (61%) mujeres. Los resultados de la encuesta PedsQL promedio fue de 77.2 sobre 100 con relación a la calidad de vida, con un rango inter cuartil (IQR) de 63.1-83.0 y una desviación estándar (DS) de 4.7. Conclusiones: La calidad de vida de pacientes pediátricos, posterior a cirugía en UNICAR en los años 2014-2017, que presentaron diagnóstico de CIV fue de 77.2%. No se logró determinar una diferencia significativa entre resultados de la encuesta PedsQL entre distintos sexos o por rango de edad. La sobrevida de los pacientes fue de 4.2 años.

Published

2021

5. The effect of preoperative nutritional status on postoperative outcomes in children undergoing surgery for congenital heart defects in San Francisco (UCSF) and Guatemala City (UNICAR)

Author

Radman, Monique, Mack, Ricardo, Barnoya, Joaquin, Castañeda, Aldo, Rosales, Monica, Azakie, Anthony, Mehta, Nilesh, Keller, Roberta, Datar, Sanjeev, Oishi, Peter, and Fineman, Jeffrey

Subjects

Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Sciences, Pediatric, Patient Safety, Cardiovascular, Clinical Research, Heart Disease, Zero Hunger, Adiposity, Biomarkers, Cardiac Surgical Procedures, Cardiotonic Agents, Child Nutrition Disorders, Child Nutritional Physiological Phenomena, Child, Preschool, Female, Guatemala, Heart Defects, Congenital, Humans, Infant, Infant Nutrition Disorders, Infant, Newborn, Length of Stay, Linear Models, Logistic Models, Male, Malnutrition, Multivariate Analysis, Natriuretic Peptide, Brain, Nutritional Status, Pilot Projects, Postoperative Complications, Prealbumin, Prospective Studies, Respiration, Artificial, Risk Factors, San Francisco, Serum Albumin, Serum Albumin, Human, Skinfold Thickness, Time Factors, Treatment Outcome, 18, 20, 21, B-type natriuretic peptide, BMI, BNP, CHD, CI, CPB, ICU, LOS, La Unidad de Cirugia Cardiovascular de Guatemala, PCICU, TSFZ, UCSF, UNICAR, University of California at San Francisco, WHO, World Health Organization, body mass index, cardiopulmonary bypass, confidence interval, congenital heart disease, intensive care unit, length of stay, pediatric cardiac intensive care unit, triceps skin-fold-for-age z score, Cardiorespiratory Medicine and Haematology, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences

Abstract

ObjectiveThe objective of this study was to determine the association between preoperative nutritional status and postoperative outcomes in children undergoing surgery for congenital heart defects (CHD).MethodsSeventy-one patients with CHD were enrolled in a prospective, 2-center cohort study. We adjusted for baseline risk differences using a standardized risk adjustment score for surgery for CHD. We assigned a World Health Organization z score for each subject's preoperative triceps skin-fold measurement, an assessment of total body fat mass. We obtained preoperative plasma concentrations of markers of nutritional status (prealbumin, albumin) and myocardial stress (B-type natriuretic peptide [BNP]). Associations between indices of preoperative nutritional status and clinical outcomes were sought.ResultsSubjects had a median (interquartile range [IQR]) age of 10.2 (33) months. In the University of California at San Francisco (UCSF) cohort, duration of mechanical ventilation (median, 19 hours; IQR, 29 hours), length of intensive care unit stay (median, 5 days; IQR 5 days), duration of any continuous inotropic infusion (median, 66 hours; IQR 72 hours), and preoperative BNP levels (median, 30 pg/mL; IQR, 75 pg/mL) were associated with a lower preoperative triceps skin-fold z score (P

Published

2014

6. Highly Efficient Targeting of EGFR-Expressing Tumor Cells with UniCAR T Cells via Target Modules Based on Cetuximab®.

Author

Jureczek, Justyna, Feldmann, Anja, Bergmann, Ralf, Arndt, Claudia, Berndt, Nicole, Koristka, Stefanie, Loureiro, Liliana Rodrigues, Mitwasi, Nicola, Hoffmann, Anja, Kegler, Alexandra, Bartsch, Tabea, and Bachmann, Michael

Subjects

*CETUXIMAB, *T cells, *LYSIS, *CHIMERIC antigen receptors, *TUMOR lysis syndrome, *CELLULAR therapy

Abstract

Introduction: Since epithelial growth factor receptor (EGFR) overexpression is linked to a variety of malignancies, it is an attractive target for immune therapy including chimeric antigen receptor (CAR)-engineered T cells. Unfortunately, CAR T cell therapy harbors the risk of severe, even life-threatening side effects. Adaptor CAR T cell platforms such as the previously described UniCAR system might be able to overcome these problems. In contrast to conventional CARs, UniCAR T cells are per se inert. Their redirection towards target cells occurs only in the presence of a tumor-specific target molecule (TM). TMs are bifunctional molecules being able to recognize a tumor-associated antigen and to cross-link the CAR T cell via a peptide epitope recognized by the UniCAR domain. Materials and Methods: Here, we compare αEGFR TMs: a nanobody (nb)-based αEGFR TM derived from the camelid αEGFR antibody 7C12 with a murine and humanized single-chain fragment variable (scFv) based on the clinically used antibody Cetuximab®. Results: In principle, both the nb- and scFv-based TM formats are able to redirect UniCAR T cells to eliminate EGFR-expressing tumor cells in an antigen-specific and TM-dependent manner. However, the scFv-based αEGFR TM was significantly superior to the nb-based TM especially with respect to lysis of tumor cells. Discussion: Improved efficiency of the scFv-based TM allowed the redirection of UniCAR T cells towards tumor cells expressing high as well as low EGFR levels in comparison to nb-based αEGFR TMs. [ABSTRACT FROM AUTHOR]

Published

2020

7. Highly Efficient Targeting of EGFR-Expressing Tumor Cells with UniCAR T Cells via Target Modules Based on Cetuximab®.

Author

Jureczek, Justyna, Feldmann, Anja, Bergmann, Ralf, Arndt, Claudia, Berndt, Nicole, Koristka, Stefanie, Loureiro, Liliana Rodrigues, Mitwasi, Nicola, Hoffmann, Anja, Kegler, Alexandra, Bartsch, Tabea, and Bachmann, Michael

Subjects

CETUXIMAB, T cells, LYSIS, CHIMERIC antigen receptors, TUMOR lysis syndrome, CELLULAR therapy

Abstract

Introduction: Since epithelial growth factor receptor (EGFR) overexpression is linked to a variety of malignancies, it is an attractive target for immune therapy including chimeric antigen receptor (CAR)-engineered T cells. Unfortunately, CAR T cell therapy harbors the risk of severe, even life-threatening side effects. Adaptor CAR T cell platforms such as the previously described UniCAR system might be able to overcome these problems. In contrast to conventional CARs, UniCAR T cells are per se inert. Their redirection towards target cells occurs only in the presence of a tumor-specific target molecule (TM). TMs are bifunctional molecules being able to recognize a tumor-associated antigen and to cross-link the CAR T cell via a peptide epitope recognized by the UniCAR domain. Materials and Methods: Here, we compare αEGFR TMs: a nanobody (nb)-based αEGFR TM derived from the camelid αEGFR antibody 7C12 with a murine and humanized single-chain fragment variable (scFv) based on the clinically used antibody Cetuximab®. Results: In principle, both the nb- and scFv-based TM formats are able to redirect UniCAR T cells to eliminate EGFR-expressing tumor cells in an antigen-specific and TM-dependent manner. However, the scFv-based αEGFR TM was significantly superior to the nb-based TM especially with respect to lysis of tumor cells. Discussion: Improved efficiency of the scFv-based TM allowed the redirection of UniCAR T cells towards tumor cells expressing high as well as low EGFR levels in comparison to nb-based αEGFR TMs. [ABSTRACT FROM AUTHOR]

Published

2020

8. Multivalent adaptor proteins specifically target NK cells carrying a universal chimeric antigen receptor to ErbB2 (HER2)-expressing cancers

Author

Pfeifer Serrahima, J., Zhang, C., Oberoi, P., Bodden, M., Röder, J., (0000-0002-1285-5052) Arndt, C., (0000-0001-5099-2448) Feldmann, A., Kiefer, A., Prüfer, M., Kühnel, I., Tonn, T., (0000-0002-8029-5755) Bachmann, M., Wels, W. S., Pfeifer Serrahima, J., Zhang, C., Oberoi, P., Bodden, M., Röder, J., (0000-0002-1285-5052) Arndt, C., (0000-0001-5099-2448) Feldmann, A., Kiefer, A., Prüfer, M., Kühnel, I., Tonn, T., (0000-0002-8029-5755) Bachmann, M., and Wels, W. S.

Abstract

Chimeric antigen receptor (CAR)-engineered immune effector cells constitute a promising approach for adoptive cancer immunotherapy. Nevertheless, on-target/off-tumor toxicity and immune escape due to antigen loss represent considerable challenges. These may be overcome by adaptor CARs that are selectively triggered by bispecific molecules that crosslink the CAR with a tumor-associated surface antigen. Here, we generated NK cells carrying a first- or second-generation universal CAR (UniCAR) and redirected them to tumor cells with so-called target modules (TMs) which harbor an ErbB2 (HER2)-specific antibody domain for target cell binding and the E5B9 peptide recognized by the UniCAR. To investigate differential effects of the protein design on activity, we developed homodimeric TMs with one, two or three E5B9 peptides per monomer, and binding domains either directly linked or separated by an IgG4 Fc domain. The adaptor molecules were expressed as secreted proteins in Expi293F cells, purified from culture supernatants and their bispecific binding to UniCAR and ErbB2 was confirmed by flow cytometry. In cell killing experiments, all tested TMs redirected NK cell cytotoxicity selectively to ErbB2-positive tumor cells. Nevertheless, we found considerable differences in the extent of specific cell killing depending on TM design and CAR composition, with adaptor proteins carrying two or three E5B9 epitopes being more effective when combined with NK cells expressing the first-generation UniCAR, while the second-generation UniCAR was more active in the presence of TMs with one E5B9 sequence. These results may have important implications for the further development of optimized UniCAR and target module combinations for cancer immunotherapy.

Published

2023

9. FLT3-directed UniCAR T-cell therapy of Acute Myeloid Leukaemia

Author

Peschke, J., (0000-0002-8733-4286) Bergmann, R., Mehnert, M., González Soto, K. E., Rodrigues Loureiro, L. R., Mitwasi, N., Kegler, A., Altmann, H., Wobus, M., Máthé, D., Szigeti, K., (0000-0001-5099-2448) Feldmann, A., Bornhäuser, M., (0000-0002-8029-5755) Bachmann, M., Fasslrinner, F., (0000-0002-1285-5052) Arndt, C., Peschke, J., (0000-0002-8733-4286) Bergmann, R., Mehnert, M., González Soto, K. E., Rodrigues Loureiro, L. R., Mitwasi, N., Kegler, A., Altmann, H., Wobus, M., Máthé, D., Szigeti, K., (0000-0001-5099-2448) Feldmann, A., Bornhäuser, M., (0000-0002-8029-5755) Bachmann, M., Fasslrinner, F., and (0000-0002-1285-5052) Arndt, C.

Abstract

Adaptor chimeric antigen receptor (CAR) T-cell therapy offers solutions for improved safety and antigen escape which represent main obstacles for the clinical translation of CAR T-cell therapy in myeloid malignancies. The adaptor CAR T-cell platform “UniCAR” is currently under early clinical investigation. Recently, first proof-of-concept of a well-tolerated, rapidly switchable, CD123-directed UniCAR T-cell product treating patients with acute myeloid leukaemia (AML) was reported. Relapsed and refractory AML is prone to a high plasticity under therapy pressure targeting one single tumour antigen. Thus, targeting of multiple tumour antigens seems to be required to achieve durable anti-tumour responses, underlining the need to further design alternative AML-specific target modules (TM) for the UniCAR platform. We here present the preclinical development of a novel FMS-like tyrosine kinase 3 (FLT3)-directed UniCAR T-cell therapy, which is highly effective for in vitro killing of both AML cell lines and primary AML samples. Furthermore, we show in vivo functionality in a murine xenograft model. PET analyses further demonstrate a short serum half-life of FLT3 TMs, which will enable a rapid on/off-switch of UniCAR T-cells. Overall, the presented preclinical data encourage the further development and clinical translation of FLT3-specific UniCAR T-cells for the therapy of AML.

Published

2023

10. A theranostic PSMA ligand for PET imaging and retargeting of T cells expressing the universal chimeric antigen receptor UniCAR

Author

Claudia Arndt, Anja Feldmann, Stefanie Koristka, Martin Schäfer, Ralf Bergmann, Nicola Mitwasi, Nicole Berndt, Dominik Bachmann, Alexandra Kegler, Marc Schmitz, Edinson Puentes-Cala, Javier Andrés Soto, Gerhard Ehninger, Jens Pietzsch, Christos Liolios, Gerd Wunderlich, Jörg Kotzerke, Klaus Kopka, and Michael Bachmann

Subjects

psma ligand, unicar, prostate cancer, immunotherapy, pet imaging, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Chimeric antigen receptor (CAR) T cells have shown impressive therapeutic potential. Due to the lack of direct control mechanisms, therapy-related adverse reactions including cytokine release- and tumor lysis syndrome can even become life-threatening. In case of target antigen expression on non-malignant cells, CAR T cells can also attack healthy tissues. To overcome such side effects, we have established a modular CAR platform termed UniCAR: UniCAR T cells per se are inert as they recognize a peptide epitope (UniCAR epitope) that is not accessible on the surface of living cells. Bifunctional adapter molecules termed target modules (TM) can cross-link UniCAR T cells with target cells. In the absence of TMs, UniCAR T cells automatically turn off. Until now, all UniCAR TMs were constructed by fusion of the UniCAR epitope to an antibody domain. To open up the wide field of low-molecular-weight compounds for retargeting of UniCAR T cells to tumor cells, and to follow in parallel the progress of UniCAR T cell therapy by PET imaging we challenged the idea to convert a PET tracer into a UniCAR-TM. For proof of concept, we selected the clinically used PET tracer PSMA-11, which binds to the prostate-specific membrane antigen overexpressed in prostate carcinoma. Here we show that fusion of the UniCAR epitope to PSMA-11 results in a low-molecular-weight theranostic compound that can be used for both retargeting of UniCAR T cells to tumor cells, and for non-invasive PET imaging and thus represents a member of a novel class of theranostics.

Published

2019

11. A theranostic PSMA ligand for PET imaging and retargeting of T cells expressing the universal chimeric antigen receptor UniCAR.

Author

Arndt, Claudia, Feldmann, Anja, Koristka, Stefanie, Schäfer, Martin, Bergmann, Ralf, Mitwasi, Nicola, Berndt, Nicole, Bachmann, Dominik, Kegler, Alexandra, Schmitz, Marc, Puentes-Cala, Edinson, Soto, Javier Andrés, Ehninger, Gerhard, Pietzsch, Jens, Liolios, Christos, Wunderlich, Gerd, Kotzerke, Jörg, Kopka, Klaus, and Bachmann, Michael

Subjects

*T cells, *CHIMERIC antigen receptors, *T cell receptors, *PROSTATE-specific membrane antigen, *PET therapy

Abstract

Chimeric antigen receptor (CAR) T cells have shown impressive therapeutic potential. Due to the lack of direct control mechanisms, therapy-related adverse reactions including cytokine release- and tumor lysis syndrome can even become life-threatening. In case of target antigen expression on non-malignant cells, CAR T cells can also attack healthy tissues. To overcome such side effects, we have established a modular CAR platform termed UniCAR: UniCAR T cells per se are inert as they recognize a peptide epitope (UniCAR epitope) that is not accessible on the surface of living cells. Bifunctional adapter molecules termed target modules (TM) can cross-link UniCAR T cells with target cells. In the absence of TMs, UniCAR T cells automatically turn off. Until now, all UniCAR TMs were constructed by fusion of the UniCAR epitope to an antibody domain. To open up the wide field of low-molecular-weight compounds for retargeting of UniCAR T cells to tumor cells, and to follow in parallel the progress of UniCAR T cell therapy by PET imaging we challenged the idea to convert a PET tracer into a UniCAR-TM. For proof of concept, we selected the clinically used PET tracer PSMA-11, which binds to the prostate-specific membrane antigen overexpressed in prostate carcinoma. Here we show that fusion of the UniCAR epitope to PSMA-11 results in a low-molecular-weight theranostic compound that can be used for both retargeting of UniCAR T cells to tumor cells, and for non-invasive PET imaging and thus represents a member of a novel class of theranostics. [ABSTRACT FROM AUTHOR]

Published

2019

12. Conventional CARs versus modular CARs.

Author

Feldmann, Anja, Arndt, Claudia, Koristka, Stefanie, Berndt, Nicole, Bergmann, Ralf, and Bachmann, Michael P.

Subjects

*CHIMERIC antigen receptors, *T cells, *TUMOR lysis syndrome

Abstract

The clinical application of immune effector cells genetically modified to express chimeric antigen receptors (CARs) has shown impressive results including complete remissions of certain malignant hematological diseases. However, their application can also cause severe side effects such as cytokine release syndrome (CRS) or tumor lysis syndrome (TLS). One limitation of currently applied CAR T cells is their lack of regulation. Especially, an emergency shutdown of CAR T cells in case of life-threatening side effects is missing. Moreover, targeting of tumor-associated antigens (TAAs) that are not only expressed on tumor cells but also on vital tissues requires the possibility of a switch allowing to repeatedly turn the activity of CAR T cells on and off. Here we summarize the development of a modular CAR variant termed universal CAR (UniCAR) system that promises to overcome these limitations of conventional CARs. [ABSTRACT FROM AUTHOR]

Published

2019

13. The UniCAR system: A modular CAR T cell approach to improve the safety of CAR T cells.

Author

Bachmann, Michael

Subjects

*T cells, *CHIMERIC antigen receptors, *TUMOR lysis syndrome, *BISPECIFIC antibodies, *DRUG side effects

Abstract

The idea to eliminate tumor cells via our own immune system is more than a hundred years old. However, a real break through came first with the development of check point inhibitors, bispecific antibodies (bsAbs) and T cells genetically modified to express Chimeric Antigen Receptors (CARs). Eventhough the clinical application of T cells equipped with CARs can lead to a complete remission, unfortunately, their application can also cause severe or even life threatening side effects as their activity can no more be adjusted once given to the patient. For targeting of tumor cells expressing tumor associated antigens (TAAs) which are not limited to tumor cells but also accessible on healthy tissues CAR T cells should not be permanently in a killing mode but be equipped with some kind of a switch whereby the activity of CAR T cells can reversely be turned "on and off ". Moreover, in case of cytokine release syndrome (CRS), tumor lysis syndrome (TLS), or other deadly side effects the possibility of an emergency shut down of the CAR T cell activity should exist. Modular CAR variants such as the UniCAR system may fulfill these requirements. [ABSTRACT FROM AUTHOR]

Published

2019

14. Theranostic CAR T cell targeting: A brief review.

Author

Arndt, Claudia, Bachmann, Michael, Bergmann, Ralf, Berndt, Nicole, Feldmann, Anja, and Koristka, Stefanie

Subjects

*T cells, *TUMOR lysis syndrome, *BISPECIFIC antibodies, *BLOOD diseases, *DRUG side effects, *T cell receptors

Abstract

More than hundred years ago, Paul Ehrlich postulated that our immune system should be able to recognize tumor cells. Just recently, the development of check point inhibitors, bispecific antibodies, and T cells genetically modified to express chimeric antigen receptors (CARs) underlines the true power of our immune system. T cells genetically modified with CARs can lead to complete remission of malignant hematologic diseases. However, they can also cause life‐threatening side effects. In case of cytokine release syndrome, tumor lysis syndrome, or deadly side effects on the central nervous system, an emergency shut down of CAR T cells is needed. Targeting of tumor‐associated antigens that are also expressed on vital tissues require a possibility to repeatedly switch the activity of CAR T cells on and off on demand and to follow the treatment by imaging. Theranostic, modular CARs such as the UniCAR system may help to overcome these problems. [ABSTRACT FROM AUTHOR]

Published

2019

15. Theranostic Antibody- and CAR-based Platform Technology for Therapy and Imaging

Author

(0000-0001-5099-2448) Feldmann, A. and (0000-0001-5099-2448) Feldmann, A.

Abstract

Theranostic Antibody- and CAR-based Platform Technology for Therapy and Imaging

Published

2022

16. Adaptor UniCAR and RevCAR platforms for flexible, switchable and combinatorial tumor targeting

Author

(0000-0001-5099-2448) Feldmann, A., Loureiro, L. R., Kegler, A., (0000-0002-1285-5052) Arndt, C., Mitwasi, N., (0000-0002-8733-4286) Bergmann, R., Koristka, S., Hoffmann, A., González Soto, K. E., Kittel-Boselli, E., Bartsch, T., Drewitz, L., (0000-0001-6921-0848) Berndt, N., Fasslrinner, F., Bornhäuser, M., (0000-0002-8029-5755) Bachmann, M., (0000-0001-5099-2448) Feldmann, A., Loureiro, L. R., Kegler, A., (0000-0002-1285-5052) Arndt, C., Mitwasi, N., (0000-0002-8733-4286) Bergmann, R., Koristka, S., Hoffmann, A., González Soto, K. E., Kittel-Boselli, E., Bartsch, T., Drewitz, L., (0000-0001-6921-0848) Berndt, N., Fasslrinner, F., Bornhäuser, M., and (0000-0002-8029-5755) Bachmann, M.

Abstract

Chimeric antigen receptor (CAR) T-cells show remarkable therapeutic effects especially in B-cell derived leukemias and lymphomas. However, clinical translation of such an innovative immunotherapeutic approach in highly heterogeneous hematological malignancies like acute myeloid leukemia (AML) or solid tumors is still challenging due to life-threatening side effects, immune escape and disease relapse. To overcome such major hurdles and to address the unmet need for further improvements in CAR therapy, we have established flexible, switchable and programmable adaptor CAR platform technologies named UniCAR and RevCAR. These modular strategies consist of T-cells engineered with adaptor CARs which are primarily inactive as they are incapable to recognize surface antigens. Universal adaptor CAR T-cells can be flexibly redirected to any tumor antigen and controlled by targeting modules (TMs) cross-linking adaptor CAR T- and tumor cells resulting in tumor cell lysis. As an advancement of UniCARs, RevCARs lack the extracellular antigen-binding moiety reducing the receptor size and facilitating the genetical modification of T-cells with several RevCARs possessing different specificity and functionality. Thus, the RevCAR platform enables combinatorial tumor targeting following Boolean logic gates. So far, we have successfully shown preclinical applicability of the UniCAR and RevCAR approaches to target hematological malignancies as well as solid tumors in a flexible and specific manner using tumor cell lines and patient-derived materials. Remarkably, efficiency and switchability of UniCAR T-cells were even proven for the first time in patients in a clinical phase I study. Furthermore, by targeting of two different tumor antigens, combinatorial OR and AND gate logic targeting according to the rules of Boolean algebra was accomplished using the RevCAR platform. These achievements have a high potential for an improved and personalized tumor immunotherapy.

Published

2022

17. Highly Efficient Targeting of EGFR-Expressing Tumor Cells with UniCAR T Cells via Target Modules Based on Cetuximab®

Author

Jureczek J, Feldmann A, Bergmann R, Arndt C, Berndt N, Koristka S, Loureiro LR, Mitwasi N, Hoffmann A, Kegler A, Bartsch T, and Bachmann M

Subjects

unicar, adaptor cars, egfr, car t cells, immunotherapy, solid tumors, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282

Abstract

Justyna Jureczek,1– 3 Anja Feldmann,3 Ralf Bergmann,3,4 Claudia Arndt,3 Nicole Berndt,3 Stefanie Koristka,3 Liliana Rodrigues Loureiro,3,5 Nicola Mitwasi,3 Anja Hoffmann,3 Alexandra Kegler,1– 3 Tabea Bartsch,3 Michael Bachmann1– 3,5,6 1German Cancer Consortium (DKTK), Dresden, Germany; 2German Cancer Research Center (DKFZ), Heidelberg, Germany; 3Department of Radioimmunology, Institute of Radiopharmaceutical Cancer Research, Helmholtz-Zentrum Dresden-Rossendorf (HZDR), Dresden, Germany; 4Department of Biophysics and Radiation Biology, Semmelweis University, Budapest, Hungary; 5National Center for Tumor Diseases (NCT), German Cancer Research Center (DKFZ), Heidelberg; Faculty of Medicine and University Hospital Carl Gustav Carus, Technische Universität Dresden, Dresden; Helmholtz-Zentrum Dresden - Rossendorf (HZDR), Dresden, Germany; 6Tumor Immunology, University Cancer Center (UCC), University Hospital Carl Gustav Carus Dresden, Technische Universität Dresden, Dresden, GermanyCorrespondence: Michael BachmannHelmholtz-Zentrum Dresden-Rossendorf e.V. Managing Director, Institute of Radiopharmaceutical Cancer Research, Bautzner Landstraße 400, Dresden 01328, GermanyTel +49 351 260 3170Fax +49 351 260 3232Email m.bachmann@hzdr.deIntroduction: Since epithelial growth factor receptor (EGFR) overexpression is linked to a variety of malignancies, it is an attractive target for immune therapy including chimeric antigen receptor (CAR)-engineered T cells. Unfortunately, CAR T cell therapy harbors the risk of severe, even life-threatening side effects. Adaptor CAR T cell platforms such as the previously described UniCAR system might be able to overcome these problems. In contrast to conventional CARs, UniCAR T cells are per se inert. Their redirection towards target cells occurs only in the presence of a tumor-specific target molecule (TM). TMs are bifunctional molecules being able to recognize a tumor-associated antigen and to cross-link the CAR T cell via a peptide epitope recognized by the UniCAR domain.Materials and Methods: Here, we compare αEGFR TMs: a nanobody (nb)-based αEGFR TM derived from the camelid αEGFR antibody 7C12 with a murine and humanized single-chain fragment variable (scFv) based on the clinically used antibody Cetuximab®.Results: In principle, both the nb- and scFv-based TM formats are able to redirect UniCAR T cells to eliminate EGFR-expressing tumor cells in an antigen-specific and TM-dependent manner. However, the scFv-based αEGFR TM was significantly superior to the nb-based TM especially with respect to lysis of tumor cells.Discussion: Improved efficiency of the scFv-based TM allowed the redirection of UniCAR T cells towards tumor cells expressing high as well as low EGFR levels in comparison to nb-based αEGFR TMs.Keywords: EGFR, UniCAR, CAR T cells, adaptor CARs, solid tumors, immunotherapy

Published

2020

18. 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

19. Conventional CARs versus modular CARs

Author

Anja Feldmann, Claudia Arndt, Ralf Bergmann, Stefanie Koristka, Michael Bachmann, and Nicole Berndt

Subjects

0301 basic medicine, Cancer Research, T-Lymphocytes, medicine.medical_treatment, Immunology, T cells, Tumor cells, TIMO XIV, Immunotherapy, Adoptive, UniCAR, BiTE, 03 medical and health sciences, 0302 clinical medicine, Antigen, Neoplasms, medicine, Humans, Immunology and Allergy, Chimeric antigen receptor, Receptors, Chimeric Antigen, business.industry, Immunotherapy, Modular design, medicine.disease, Tumor lysis syndrome, Cytokine release syndrome, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Focussed Research Review, Cancer research, Car t cells, business, human activities

Abstract

The clinical application of immune effector cells genetically modified to express chimeric antigen receptors (CARs) has shown impressive results including complete remissions of certain malignant hematological diseases. However, their application can also cause severe side effects such as cytokine release syndrome (CRS) or tumor lysis syndrome (TLS). One limitation of currently applied CAR T cells is their lack of regulation. Especially, an emergency shutdown of CAR T cells in case of life-threatening side effects is missing. Moreover, targeting of tumor-associated antigens (TAAs) that are not only expressed on tumor cells but also on vital tissues requires the possibility of a switch allowing to repeatedly turn the activity of CAR T cells on and off. Here we summarize the development of a modular CAR variant termed universal CAR (UniCAR) system that promises to overcome these limitations of conventional CARs.

Published

2019

20. The UniCAR system: A modular CAR T cell approach to improve the safety of CAR T cells

Author

Michael Bachmann

Subjects

0301 basic medicine, Bispecific antibody, T-Lymphocytes, medicine.medical_treatment, Immunology, T cells, T-Cell Antigen Receptor Specificity, Immunotherapy, Adoptive, Autoimmune Diseases, UniCAR, BiTE, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigens, Neoplasm, medicine, Animals, Humans, Immunology and Allergy, Chimeric antigen receptor, Receptors, Chimeric Antigen, business.industry, Immunotherapy, Modular design, medicine.disease, Tumor lysis syndrome, Cytokine release syndrome, 030104 developmental biology, Cancer research, Car t cells, Cytokine Release Syndrome, business, 030215 immunology

Abstract

The idea to eliminate tumor cells via our own immune system is more than a hundred years old. However, a real break through came first with the development of check point inhibitors, bispecific antibodies (bsAbs) and T cells genetically modified to express Chimeric Antigen Receptors (CARs). Eventhough the clinical application of T cells equipped with CARs can lead to a complete remission, unfortunately, their application can also cause severe or even life threatening side effects as their activity can no more be adjusted once given to the patient. For targeting of tumor cells expressing tumor associated antigens (TAAs) which are not limited to tumor cells but also accessible on healthy tissues CAR T cells should not be permanently in a killing mode but be equipped with some kind of a switch whereby the activity of CAR T cells can reversely be turned "on and off ". Moreover, in case of cytokine release syndrome (CRS), tumor lysis syndrome (TLS), or other deadly side effects the possibility of an emergency shut down of the CAR T cell activity should exist. Modular CAR variants such as the UniCAR system may fulfill these requirements.

Published

2019

21. Theranostic CAR T cell targeting: A brief review

Author

Arndt, C., Bachmann, M., Bergmann, R., Berndt, N., Feldmann, A., Koristka, S., Arndt, C., Bachmann, M., Bergmann, R., Berndt, N., Feldmann, A., and Koristka, S.

Abstract

More than 100 years ago Paul Ehrlich postulated that our immun system should be able to eliminate tumor cells. Just recently, the development of check point inhibitors, bispecific antibodies, and T cells genetically modified to express chimeric antigen receptors (CARs) underlines the true power of our immune system. T cells genetically modified with CARs can lead to complete remission of malignant hematologic diseases. However, they can also cause life-threatening side effects. In case of cytokine release syndrome, tumor lysis syndrome, or deadly side effects on the central nervous system, an emergency shut down of CAR T cells is needed. Targeting of tumor-associated antigens that are also expressed on vital tissues require a possibility to repeatedly switch the activity of CAR T cells on and off on demand and to follow the treatment by imaging. Theranostic, modular CARs such as the UniCAR system may help to overcome these problems.

Published

2019

22. A theranostic PSMA ligand for PET imaging and retargeting of T cells expressing the universal chimeric antigen receptor UniCAR

Author

(0000-0002-1285-5052) Arndt, C., (0000-0001-5099-2448) Feldmann, A., Koristka, S., Schäfer, M., (0000-0002-8733-4286) Bergmann, R., Metwasi, N., (0000-0001-6921-0848) Berndt, N., Bachmann, D., Kegler, A., Schmitz, M., Puentes-Cala, E., Soto, J. A., Ehninger, G., Pietzsch, J., Liolios, C., Wunderlich, G., Kotzerke, J., (0000-0003-4846-1271) Kopka, K., (0000-0002-8029-5755) Bachmann, M., (0000-0002-1285-5052) Arndt, C., (0000-0001-5099-2448) Feldmann, A., Koristka, S., Schäfer, M., (0000-0002-8733-4286) Bergmann, R., Metwasi, N., (0000-0001-6921-0848) Berndt, N., Bachmann, D., Kegler, A., Schmitz, M., Puentes-Cala, E., Soto, J. A., Ehninger, G., Pietzsch, J., Liolios, C., Wunderlich, G., Kotzerke, J., (0000-0003-4846-1271) Kopka, K., and (0000-0002-8029-5755) Bachmann, M.

Abstract

Chimeric antigen receptor (CAR) T cells have shown impressive therapeutic potential. Due to the lack of direct control mechanisms, therapy-related adverse reactions including cytokine release- and tumor lysis syndrome can even become life-threatening. In case of target antigen expression on non-malignant cells, CAR T cells can also attack healthy tissues. To overcome such side effects, we have established a modular CAR platform termed UniCAR: UniCAR T cells per se are inert as they recognize a peptide epitope (UniCAR epitope) that is not accessible on the surface of living cells. Bifunctional adapter molecules termed target modules (TM) can cross-link UniCAR T cells with target cells. In the absence of TMs, UniCAR T cells automatically turn off. Until now, all UniCAR TMs were constructed by fusion of the UniCAR epitope to an antibody domain. To open up the wide field of low-molecular weight compounds for retargeting of UniCAR T cells to tumor cells, and to follow in parallel the progress of UniCAR T cell therapy by PET imaging we challenged the idea to convert a PET tracer into a UniCAR-TM. For proof of concept, we selected the clinically used PET tracer PSMA-11, which binds to the prostate-specific membrane antigen overexpressed in prostate carcinoma. Here we show that fusion of the UniCAR epitope to PSMA-11 results in a low-molecular weight theranostic compound that can be used for both retargeting of UniCAR T cells to tumor cells, and for non-invasive PET imaging and thus represents a member of a novel class of theranostics.

Published

2019

23. The UniCAR system: A modular CAR T cell approach to improve the safety of CAR T cells

Author

(0000-0002-8029-5755) Bachmann, M. and (0000-0002-8029-5755) Bachmann, M.

Abstract

The idea to eliminate tumor cells via our own immune system is more than a hundred years old. However, a real break through came first with the development of check point inhibitors, bispecific antibodies (bsAbs) and T cells genetically modified to express Chimeric Antigen Receptors (CARs). Eventhough the clinical application of T cells equipped with CARs can lead to a complete remission, unfortunately, their application can also cause severe or even life threatening side effects as their activity can no more be adjusted once given to the patient. For targeting of tumor cells expressing tumor associated antigens (TAAs) which are not limited to tumor cells but also accessible on healthy tissues CAR T cells should not be permanently in a killing mode but be equipped with some kind of a switch whereby the activity of CAR T cells can reversely be turned “on and off “. Moreover, in case of cytokine release syndrome (CRS), tumor lysis syndrome (TLS), or other deadly side effects the possibility of an emergency shut down of the CAR T cell activity should exist. Modular CAR variants such as the UniCAR system may fulfill these requirements.

Published

2019

24. Conventional CARs versus modular CARs

Author

(0000-0001-5099-2448) Feldmann, A., (0000-0002-1285-5052) Arndt, C., Koristka, S., (0000-0001-6921-0848) Berndt, N., (0000-0002-8733-4286) Bergmann, R., (0000-0002-8029-5755) Bachmann, M., (0000-0001-5099-2448) Feldmann, A., (0000-0002-1285-5052) Arndt, C., Koristka, S., (0000-0001-6921-0848) Berndt, N., (0000-0002-8733-4286) Bergmann, R., and (0000-0002-8029-5755) Bachmann, M.

Abstract

The clinical application of immune effector cells genetically modified to express chimeric antigen receptors (CARs) has shown impressive results including complete remissions of certain malignant hematological diseases. However, their application can also cause severe side effects such as cytokine release syndrome (CRS) or tumor lysis syndrome (TLS). One limitation of currently applied CAR T cells is their lack of regulation. Especially, an emergency shutdown of CAR T cells in case of life-threatening side effects is missing. Moreover, targeting of tumor-associated antigens (TAAs) that are not only expressed on tumor cells but also on vital tissues requires the possibility of a switch allowing to repeatedly turn the activity of CAR T cells on and off. Here we summarize the development of a modular CAR variant termed universal CAR (UniCAR) system that promises to overcome these limitations of conventional CARs.

Published

2019

25. SYSTÉM VNITROPODNIKOVÉ LOGISTIKY

Author

Jaromír Široký

Subjects

systém, vnitropodniková logistika, UNICAR, Railroad engineering and operation, TF1-1620, Industrial engineering. Management engineering, T55.4-60.8

Abstract

Příspěvek se zabývá optimalizací logistických a distribučních procesů v různých výrobních podnicích a institucích. Je zde popsán systém vnitropodnikové logistiky Unicar. Spočívá v dopravě vozidel s kontejnery po speciální kolejové dráze a pomáhá tak při doručování zásob a jiných materiálů v podniku.

Published

2006

26. A theranostic PSMA ligand for PET imaging and retargeting of T cells expressing the universal chimeric antigen receptor UniCAR

Author

Dominik Bachmann, Marc Schmitz, Klaus Kopka, Gerhard Ehninger, Gerd Wunderlich, Javier Andrés Soto, Ralf Bergmann, Anja Feldmann, Martin Schäfer, Nicole Berndt, Edinson Puentes-Cala, Alexandra Kegler, Jörg Kotzerke, Jens Pietzsch, Nicola Mitwasi, Claudia Arndt, Christos Liolios, Stefanie Koristka, Michael Bachmann, and Taylor & Francis Group

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, medicine.medical_treatment, T cell, Immunology, PSMA ligand, PET imaging, lcsh:RC254-282, Epitope, UniCAR, psma ligand, unicar, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, medicine, Immunology and Allergy, Original Research, biology, Chemistry, Immunotherapy, prostate cancer, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, Chimeric antigen receptor, Cell biology, 030104 developmental biology, Cytokine, medicine.anatomical_structure, Oncology, pet imaging, 030220 oncology & carcinogenesis, Retargeting, biology.protein, immunotherapy, Antibody, lcsh:RC581-607

Abstract

Digital, Chimeric antigen receptor (CAR) T cells have shown impressive therapeutic potential. Due to the lack of direct control mechanisms, therapy-related adverse reactions including cytokine release- and tumor lysis syndrome can even become life-threatening. In case of target antigen expression on non-malignant cells, CAR T cells can also attack healthy tissues. To overcome such side effects, we have established a modular CAR platform termed UniCAR: UniCAR T cells per se are inert as they recognize a peptide epitope (UniCAR epitope) that is not accessible on the surface of living cells. Bifunctional adapter molecules termed target modules (TM) can cross-link UniCAR T cells with target cells. In the absence of TMs, UniCAR T cells automatically turn off. Until now, all UniCAR TMs were constructed by fusion of the UniCAR epitope to an antibody domain. To open up the wide field of low-molecular-weight compounds for retargeting of UniCAR T cells to tumor cells, and to follow in parallel the progress of UniCAR T cell therapy by PET imaging we challenged the idea to convert a PET tracer into a UniCAR-TM. For proof of concept, we selected the clinically used PET tracer PSMA-11, which binds to the prostate-specific membrane antigen overexpressed in prostate carcinoma. Here we show that fusion of the UniCAR epitope to PSMA-11 results in a low-molecular-weight theranostic compound that can be used for both retargeting of UniCAR T cells to tumor cells, and for non-invasive PET imaging and thus represents a member of a novel class of theranostics., 1 ed.

Published

2019

27. Influence of Histidine-tag on immunotherapeutic and diagnostic properties of anti-PSCA target modules

Author

Jureczek, J., Bergmann, R., Berndt, N., Albert, S., Koristka, S., Arndt, C., Steinbach, J., Bachmann, M., Feldmann, A., Jureczek, J., Bergmann, R., Berndt, N., Albert, S., Koristka, S., Arndt, C., Steinbach, J., Bachmann, M., and Feldmann, A.

Abstract

Antibodies (Abs) and their recombinant derivatives play an increasing role in tumor therapy and diagnostic imaging. The theranostic target modules (TMs) recently developed by us can be used for individualized and precise cancer immunotherapy and at the same time as radiotracers for tumor imaging. The TMs consist of an antigen binding moiety that binds to the prostate stem cell antigen (PSCA) on the tumor cell surface and present the peptide epitope E5B9. Via E5B9 the TMs can retarget human T cells that are genetically modified with universal anti-E5B9 chimeric antigen receptors (UniCARs) towards the tumor cells. The cross-linkage of UniCAR T cells and tumor cells via the TM results in T cell activation and tumor cell killing. This immunotherapeutic approach was shown as an inducible CAR platform technology that can be used for the treatment of leukemic as well as solid cancers. This technic has an intrinsic emergency brake: The short half-life of the TMs in vivo allows a fast switch off of the UniCAR system. In detail, UniCAR T cells per se are inactive because their UniCARs do not recognize an antigen on the cell surface. Only in the presence of tumor-bound TMs UniCAR T cells can be redirected to tumor cells and turned on. But they are switched off when the application of TMs is stopped and their concentration is too low to activate UniCAR T cells what also becomes particularly relevant in case of side effects occur in the patients. TMs cannot only be used as a therapeutic drug but also as a diagnostic tool for tumor imaging. For this purpose TMs can be modified with a bifunctional chelator. After conjugation they can be labeled with radiometals like 64Cu2+ or 68Ga3+ and used as an imaging tracer for PET analysis. Usually our TMs contain a tag of six histidine residues (His6-tag) at the C-terminus. The His6-tag is used for convenient purification by immobilized metal ion affinity chromatography and detection of the TMs. However the His6-tag may affect PK and biodis

Published

2018

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

Author

Loff S, Dietrich J, Meyer JE, Riewaldt J, Spehr J, von Bonin M, Gründer C, Swayampakula M, Franke K, Feldmann A, Bachmann M, Ehninger G, Ehninger A, and Cartellieri M

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)., (© 2020 The Author(s).)

Published

2020