Your search keyword '"Rabsteyn, Armin"' showing total 6 results

1. Novel adapter CAR-T cell technology for precisely controllable multiplex cancer targeting.

Author

Seitz, Christian M., Mittelstaet, Joerg, Atar, Daniel, Hau, Jana, Reiter, Selina, Illi, Clara, Kieble, Verena, Engert, Fabian, Drees, Britta, Bender, Giulia, Krahl, Ann-Christin, Knopf, Philipp, Schroeder, Sarah, Paulsen, Nikolas, Rokhvarguer, Alexander, Scheuermann, Sophia, Rapp, Elena, Mast, Anna-Sophia, Rabsteyn, Armin, and Schleicher, Sabine

Subjects

*CELL surface antigens, *CHIMERIC antigen receptors, *IMMUNE response, *CANCER treatment

Abstract

Chimeric antigen receptor (CAR)-T therapy holds great promise to sustainably improve cancer treatment. However, currently, a broad applicability of CAR-T cell therapies is hampered by limited CAR-T cell versatility and tractability and the lack of exclusive target antigens to discriminate cancerous from healthy tissues. To achieve temporal and qualitative control on CAR-T function, we engineered the Adapter CAR (AdCAR) system. AdCAR-T are redirected to surface antigens via biotin-labeled adapter molecules in the context of a specific linker structure, referred to as Linker-Label-Epitope. AdCAR-T execute highly specific and controllable effector function against a multiplicity of target antigens. In mice, AdCAR-T durably eliminate aggressive lymphoma. Importantly, AdCAR-T might prevent antigen evasion by combinatorial simultaneous or sequential targeting of multiple antigens and are capable to identify and differentially lyse cancer cells by integration of adapter molecule-mediated signals based on multiplex antigen expression profiles. In consequence the AdCAR technology enables controllable, flexible, combinatorial, and selective targeting. [ABSTRACT FROM AUTHOR]

Published

2021

2. Defibrotide for the Treatment of Pediatric Inflammatory Multisystem Syndrome Temporally Associated With Severe Acute Respiratory Syndrome Coronavirus 2 Infection in 2 Pediatric Patients.

Author

Lang, Peter, Eichholz, Thomas, Bakchoul, Tamam, Streiter, Monika, Petrasch, Maurice, Bösmüller, Hans, Klein, Reinhild, Rabsteyn, Armin, Lang, Anne-Marie, Adams, Constantin, Klingel, Karin, Gessner, Michaela, Rosenberger, Peter, Ruef, Peter, and Handgretinger, Rupert

Subjects

*MULTISYSTEM inflammatory syndrome in children, *PEDIATRICS, *SARS disease

Abstract

The pediatric inflammatory multisystem syndrome temporally associated with severe acute respiratory syndrome coronavirus 2 infection is a severe complication of coronavirus disease 2019. Since impaired coagulation and thrombosis/endotheliitis are suspected pathomechanisms, we treated 2 patients with defibrotide, a profibrinolytic, antithrombotic, antiinflammatory oligonucleotide. Symptoms resolved during treatment. Moreover, coagulation parameters indicating hypofibrinolysis and complement activation normalized. The pediatric inflammatory multisystem syndrome temporally associated with severe acute respiratory syndrome coronavirus 2 infection is a severe complication of coronavirus disease 2019. Since impaired coagulation and thrombosis/endotheliitis are suspected pathomechanisms, 2 patients received defibrotide, a profibrinolytic, antithrombotic, antiinflammatory oligonucleotide. Symptoms resolved and hypofibrinolysis/complement activation normalized during treatment. [ABSTRACT FROM AUTHOR]

Published

2020

3. Low mutational load in pediatric medulloblastoma still translates into neoantigens as targets for specific T-cell immunotherapy.

Author

Blaeschke, Franziska, Paul, Milan Cedric, Schuhmann, Martin Ulrich, Rabsteyn, Armin, Schroeder, Christopher, Casadei, Nicolas, Matthes, Jakob, Mohr, Christopher, Lotfi, Ramin, Wagner, Beate, Kaeuferle, Theresa, Feucht, Judith, Willier, Semjon, Handgretinger, Rupert, StevanoviĆ, Stefan, Lang, Peter, and Feuchtinger, Tobias

Subjects

*GENETIC load, *MEDULLOBLASTOMA, *CYTOTOXIC T cells, *TUMOR necrosis factors, *HLA histocompatibility antigens, *CANCER vaccines

Abstract

Medulloblastoma is the most common malignant brain tumor in childhood and adolescence. Although some patients present with distinct genetic alterations, such as mutated TP53 or MYC amplification, pediatric medulloblastoma is a tumor entity with minimal mutational load and low immunogenicity. We identified tumor-specific mutations using next-generation sequencing of medulloblastoma DNA and RNA derived from primary tumor samples from pediatric patients. Tumor-specific mutations were confirmed using deep sequencing and in silico analyses predicted high binding affinity of the neoantigen-derived peptides to the patients' human leukocyte antigen molecules. Tumor-specific peptides were synthesized and used to induce a de novo T-cell response characterized by interferon gamma and tumor necrosis factor alpha release of CD8+ cytotoxic T cells in vitro. Despite low mutational tumor burden, at least two immunogenic tumor-specific peptides were identified in each patient. T cells showed a balanced CD4/CD8 ratio and mostly effector memory phenotype. Induction of a CD8-specific T-cell response was achieved for the neoepitopes derived from Histidine Ammonia-Lyase (HAL), Neuraminidase 2 (NEU2), Proprotein Convertase Subtilisin (PCSK9), Programmed Cell Death 10 (PDCD10), Supervillin (SVIL) and tRNA Splicing Endonuclease Subunit 54 (TSEN54) variants. Detection of patient-specific, tumor-derived neoantigens confirms that even in tumors with low mutational load a molecular design of targets for specific T-cell immunotherapy is possible. The identified neoantigens may guide future approaches of adoptive T-cell transfer, transgenic T-cell receptor transfer or tumor vaccination. [ABSTRACT FROM AUTHOR]

Published

2019

4. CD34+ selected stem cell boosts can improve poor graft function after paediatric allogeneic stem cell transplantation.

Author

Mainardi, Chiara, Ebinger, Martin, Enkel, Sigrid, Feuchtinger, Tobias, Teltschik, Heiko‐Manuel, Eyrich, Matthias, Schumm, Michael, Rabsteyn, Armin, Schlegel, Patrick, Seitz, Christian, Schwarze, Carl‐Phillip, Müller, Ingo, Greil, Johann, Bader, Peter, Schlegel, Paul‐Gerhardt, Martin, David, Holzer, Ursula, Döring, Michaela, Handgretinger, Rupert, and Lang, Peter

Subjects

*STEM cell transplantation, *NEUTROPHILS, *HEMATOLOGY, *LYMPHOCYTES, *ERYTHROCYTES

Abstract

Poor graft function ( PGF) is a severe complication of haematopoietic stem cell transplantation ( HSCT) and administration of donor stem cell boosts ( SCBs) represents a therapeutic option. We report 50 paediatric patients with PGF who received 61 boosts with CD34+ selected peripheral blood stem cells ( PBSC) after transplantation from matched unrelated ( n = 25) or mismatched related ( n = 25) donors. Within 8 weeks, a significant increase in median neutrophil counts (0·6 vs. 1·516 × 109/l, P < 0·05) and a decrease in red blood cell and platelet transfusion requirement (median frequencies 1 and 7 vs. 0, P < 0·0001 and <0·001), were observed, and 78·8% of patients resolved one or two of their cytopenias. 36·5% had a complete haematological response. Median lymphocyte counts for CD3+, CD3+ CD4+, CD19+ and CD56+ increased 8·3-, 14·2-, 22.- and 1·6-fold. The rate of de novo acute graft-versus-host disease (Gv HD) grade I-III was only 6% and resolved completely. No Gv HD grade IV or chronic Gv HD occurred. Patients who responded to SCB displayed a trend toward better overall survival ( OS) ( P = 0·07). Thus, administration of CD34+ selected SCBs from alternative donors is safe and effective. Further studies are warranted to clarify the impact on immune reconstitution and survival. [ABSTRACT FROM AUTHOR]

Published

2018

5. The immunopeptidomic landscape of ovarian carcinomas.

Author

Schuster, Heiko, Peper, Janet K., Bösmüller, Hans-Christian, Röhle, Kevin, Backert, Linus, Bilich, Tatjana, Ney, Britta, Löffler, Markus W., Kowalewski, Daniel J., Trautwein, Nico, Rabsteyn, Armin, Engler, Tobias, Braun, Sabine, Haen, Sebastian P., Walz, Juliane S., Schmid-Horch, Barbara, Brucker, Sara Y., Wallwiener, Diethelm, Kohlbacher, Oliver, and Falko Fend

Subjects

*OVARIAN epithelial cancer, *IMMUNOTHERAPY, *MUCIN genetics, *MESOTHELIN, *CANCER cells, *CANCER treatment

Abstract

Immunotherapies, particularly checkpoint inhibitors, have set off a revolution in cancer therapy by releasing the power of the immune system. However, only little is known about the antigens that are essentially presented on cancer cells, capable of exposing them to immune cells. Large-scale HLA ligandome analysis has enabled us to exhaustively characterize the immunopeptidomic landscape of epithelial ovarian cancers (EOCs). Additional comparative profiling with the immunopeptidome of a variety of benign sources has unveiled a multitude of ovarian cancer antigens (MUC16, MSLN, LGALS1, IDO1, KLK10) to be presented by HLA class I and class II molecules exclusively on ovarian cancer cells. Most strikingly, ligands derived from mucin 16 and mesothelin, a molecular axis of prognostic importance in EOC, are prominent in a majority of patients. Differential gene-expression analysis has allowed us to confirm the relevance of these targets for EOC and further provided important insights into the relationship between gene transcript levels and HLA ligand presentation. [ABSTRACT FROM AUTHOR]

Published

2017

6. An open-source computational and data resource to analyze digital maps of immunopeptidomes.

Author

Caron, Etienne, Espona, Lucia, Kowalewski, Daniel J., Schuster, Heiko, Ternette, Nicola, Alpízar, Adán, Schittenhelm, Ralf B., Ramarathinam, Sri H., Lindestam Arlehamn, Cecilia S., Ching Chiek Koh, Gillet, Ludovic C., Rabsteyn, Armin, Navarro, Pedro, Sangtae Kim, Lam, Henry, Sturm, Theo, Marcilla, Miguel, Sette, Alessandro, Campbell, David S., and Deutsch, Eric W.

Subjects

*PEPTIDES, *HLA histocompatibility antigens

Abstract

The article presents the study that explores on the community-based efforts in developing robust platform that will be used in the quantitative and reproducible measurement of peptides that are presented by the human leukocyte antigen (HLA) in Switzerland.

Published

2015