Your search keyword '"Loreen Sophie, Rudek"' showing total 3 results

1. Generation of an NFκB-Driven Alpharetroviral 'All-in-One' Vector Construct as a Potent Tool for CAR NK Cell Therapy

Author

Loreen Sophie Rudek, Katharina Zimmermann, Melanie Galla, Johann Meyer, Johannes Kuehle, Andriana Stamopoulou, Daniel Brand, I. Erol Sandalcioglu, Belal Neyazi, Thomas Moritz, Claudia Rossig, Bianca Altvater, Christine S. Falk, Hinrich Abken, Michael Alexander Morgan, and Axel Schambach

Subjects

immunotherapy, NK cells, chimeric antigen receptor (CAR), tumor microenvironment, immunomodulatory cytokines, alpharetroviral vectors, Immunologic diseases. Allergy, RC581-607

Abstract

Immune cell therapeutics are increasingly applied in oncology. Especially chimeric antigen receptor (CAR) T cells are successfully used to treat several B cell malignancies. Efforts to engineer CAR T cells for improved activity against solid tumors include co-delivery of pro-inflammatory cytokines in addition to CARs, via either constitutive cytokine expression or inducible cytokine expression triggered by CAR recognition of its target antigen—so-called “T cells redirected for universal cytokine-mediated killing” (TRUCKs) or fourth-generation CARs. Here, we tested the hypothesis that TRUCK principles could be expanded to improve anticancer functions of NK cells. A comparison of the functionality of inducible promoters responsive to NFAT or NFκB in NK cells showed that, in contrast to T cells, the inclusion of NFκB-responsive elements within the inducible promoter construct was essential for CAR-inducible expression of the transgene. We demonstrated that GD2CAR-specific activation induced a tight NFκB-promoter-driven cytokine release in NK-92 and primary NK cells together with an enhanced cytotoxic capacity against GD2+ target cells, also shown by increased secretion of cytolytic cytokines. The data demonstrate biologically relevant differences between T and NK cells that are important when clinically translating the TRUCK concept to NK cells for the treatment of solid malignancies.

Published

2021

2. Design and Characterization of an 'All-in-One' Lentiviral Vector System Combining Constitutive Anti-GD2 CAR Expression and Inducible Cytokines

Author

Thomas Moritz, Christina Kloth, Johannes Kuehle, Belal Neyazi, Katharina Zimmermann, Loreen Sophie Rudek, Britta Eiz-Vesper, Claudia Rossig, I. Erol Sandalcioglu, Michael A. Morgan, Axel Schambach, Hinrich Abken, Anna Christina Dragon, Johann Meyer, Bianca Altvater, and Melanie Galla

Subjects

0301 basic medicine, gd2car, Cancer Research, NFAT, Transgene, medicine.medical_treatment, lcsh:RC254-282, Viral vector, 03 medical and health sciences, 0302 clinical medicine, medicine, Tumor microenvironment, inducible cytokines, TRUCK, Chemistry, Monocyte, “all-in-one” lentiviral vector, glioblastoma, IL18, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Chimeric antigen receptor, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Cytokine, Oncology, 030220 oncology & carcinogenesis, Interleukin 12, IL12, human activities, GD2CAR

Abstract

Genetically modified T cells expressing chimeric antigen receptors (CARs) so far have mostly failed in the treatment of solid tumors owing to a number of limitations, including an immunosuppressive tumor microenvironment and insufficient CAR T cell activation and persistence. Next-generation approaches using CAR T cells that secrete transgenic immunomodulatory cytokines upon CAR signaling, known as TRUCKs (&ldquo, T cells redirected for universal cytokine-mediated killing&rdquo, ), are currently being explored. As TRUCKs were engineered by the transduction of T cells with two separate vectors, we developed a lentiviral modular &ldquo, all-in-one&rdquo, vector system that combines constitutive CAR expression and inducible nuclear factor of activated T cells (NFAT)-driven transgene expression for more efficient production of TRUCKs. Activation of the GD2-specific CAR via GD2+ target cells induced NFAT promoter-driven cytokine release in primary human T cells, and indicated a tight linkage of CAR-specific activation and transgene expression that was further improved by a modified NFATsyn promoter. As proof-of-concept, we showed that T cells containing the &ldquo, vector system secrete the immunomodulatory cytokines interleukin (IL)12 or IL18 upon co-cultivation with primary human GD2+ tumor cells, resulting in enhanced effector cell properties and increased monocyte recruitment. This highlights the potential of our system to simplify application of TRUCK-modified T cells in solid tumor therapy.

Published

2020

3. Design and Characterization of an 'All-in-One' Lentiviral Vector System Combining Constitutive Anti-G

Author

Katharina, Zimmermann, Johannes, Kuehle, Anna Christina, Dragon, Melanie, Galla, Christina, Kloth, Loreen Sophie, Rudek, I Erol, Sandalcioglu, Belal, Neyazi, Thomas, Moritz, Johann, Meyer, Claudia, Rossig, Bianca, Altvater, Britta, Eiz-Vesper, Michael Alexander, Morgan, Hinrich, Abken, and Axel, Schambach

Subjects

inducible cytokines, TRUCK, NFAT, “all-in-one” lentiviral vector, glioblastoma, IL18, IL12, human activities, GD2CAR, Article

Abstract

Genetically modified T cells expressing chimeric antigen receptors (CARs) so far have mostly failed in the treatment of solid tumors owing to a number of limitations, including an immunosuppressive tumor microenvironment and insufficient CAR T cell activation and persistence. Next-generation approaches using CAR T cells that secrete transgenic immunomodulatory cytokines upon CAR signaling, known as TRUCKs (“T cells redirected for universal cytokine-mediated killing”), are currently being explored. As TRUCKs were engineered by the transduction of T cells with two separate vectors, we developed a lentiviral modular “all-in-one” vector system that combines constitutive CAR expression and inducible nuclear factor of activated T cells (NFAT)-driven transgene expression for more efficient production of TRUCKs. Activation of the GD2-specific CAR via GD2+ target cells induced NFAT promoter-driven cytokine release in primary human T cells, and indicated a tight linkage of CAR-specific activation and transgene expression that was further improved by a modified NFATsyn promoter. As proof-of-concept, we showed that T cells containing the “all-in-one” vector system secrete the immunomodulatory cytokines interleukin (IL)12 or IL18 upon co-cultivation with primary human GD2+ tumor cells, resulting in enhanced effector cell properties and increased monocyte recruitment. This highlights the potential of our system to simplify application of TRUCK-modified T cells in solid tumor therapy.

Published

2019