Research Papers:
Development of novel target modules for retargeting of UniCAR T cells to GD2 positive tumor cells
PDF | HTML | Supplementary Files | How to cite
Metrics: PDF 1761 views | HTML 5213 views | ?
Abstract
Nicola Mitwasi1,*, Anja Feldmann2,*, Ralf Bergmann2,*, Nicole Berndt3,*, Claudia Arndt2, Stefanie Koristka2, Alexandra Kegler2, Justyna Jureczek1, Anja Hoffmann2, Armin Ehninger4, Marc Cartellieri5, Susann Albert1, Claudia Rossig6, Gerhard Ehninger3,7,8, Jens Pietzsch2,9, Jörg Steinbach2,3,8,9 and Michael Bachmann1,2,3,7,8
1University Cancer Center (UCC) ‘Carl Gustav Carus’ TU Dresden, Tumor Immunology, Dresden, Germany
2Helmholtz-Zentrum Dresden-Rossendorf (HZDR), Institute of Radiopharmaceutical Cancer Research, Dresden, Germany
3German Cancer Consortium (DKTK), partner site Dresden, and German Cancer Research Center (DKFZ), Heidelberg, Germany
4GEMoaB Monoclonals GmbH, Dresden, Germany
5Cellex Patient Treatment GmbH, Dresden, Germany
6Department of Pediatric Hematology and Oncology, University Children´s Hospital Münster, Münster, Germany
7Medical Clinic and Policlinic I, University Hospital ‘Carl Gustav Carus’, TU Dresden, Dresden, Germany
8National Center for Tumor Diseases (NCT), Dresden, ‘Carl Gustav Carus’ TU Dresden, Dresden, Germany
9Department of Chemistry and Food Chemistry, School of Science, ‘Carl Gustav Carus’ TU Dresden, Germany
*These authors contributed equally first to this work
Correspondence to:
Michael Bachmann, email: [email protected]
Keywords: immunotherapy, CAR T cells
Received: June 13, 2017 Accepted: August 25, 2017 Published: September 18, 2017
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.
All site content, except where otherwise noted, is licensed under a Creative Commons Attribution 4.0 License.
PII: 21017