Tumor-specific T cell activation by recombinant immunoreceptors: CD3 zeta signaling and CD28 costimulation are simultaneously required for efficient IL-2 secretion and can be integrated into one combined CD28/CD3 zeta signaling receptor molecule.

6533b7dafe1ef96bd126e134

RESEARCH PRODUCT

Tumor-specific T cell activation by recombinant immunoreceptors: CD3 zeta signaling and CD28 costimulation are simultaneously required for efficient IL-2 secretion and can be integrated into one combined CD28/CD3 zeta signaling receptor molecule.

Claudia Heuser Thomas Marquardt Barbara Seliger Loretta Usai Anja Wieczarkowiecz C Pohl Andreas Hombach Hinrich Abken

subject

CD4-Positive T-Lymphocytes CD3 Complex T cell CD3 T-Lymphocytes Immunology Epitopes T-Lymphocyte chemical and pharmacologic phenomena Biology CD8-Positive T-Lymphocytes Major histocompatibility complex Lymphocyte Activation Transfection Epitope Antigen CD28 Antigens Antigens Neoplasm medicine Tumor Cells Cultured Immunology and Allergy Humans Receptors Immunologic Receptor Receptors IgG CD28 hemic and immune systems Molecular biology Coculture Techniques Recombinant Proteins Cell biology Carcinoembryonic Antigen medicine.anatomical_structure biology.protein B7-1 Antigen Interleukin-2 CD8 Signal Transduction

description

Abstract Recombinant immunoreceptors with specificity for the carcinoembryonic Ag (CEA) can redirect grafted T cells to a MHC/Ag-independent antitumor response. To analyze receptor-mediated cellular activation in the context of CD28 costimulation, we generated: 1) CEA+ colorectal tumor cells that express simultaneously B7-1 and B7-2, and 2) CEA-specific immunoreceptors that harbor intracellularly the signaling moities either of CD28 (BW431/26-scFv-Fc-CD28), CD3ζ (BW431/26-scFv-Fc-CD3ζ), or FcεRIγ (BW431/26-scFv-Fc-γ). By retroviral gene transfer, we grafted activated T cells from the peripheral blood with these immunoreceptors. T cells that express the FcεRIγ or CD3ζ signaling receptor lysed specifically CEA+ tumor cells and secreted high amounts of IFN-γ upon receptor cross-linking, whereas anti-CEA-CD28 receptor-grafted T cells did not, indicating that CD28 signaling alone is not sufficient for efficient T cell activation. CD28 costimulation did not affect cytolysis by T cells equipped with γ- or ζ-signaling receptors, but enhanced both IFN-γ secretion and proliferation. CD28 costimulation, however, was required for efficient IL-2 secretion of anti-CEA-γ receptor-grafted T cells. Both purified CD4+ and CD8+ T cells grafted with immunoreceptors required CD28 costimulation for complete T cell activation. We integrated both CD28 and CD3ζ signaling domains into one combined immunoreceptor molecule (BW431/26-scFv-Fc-CD28/CD3ζ) with dual signaling properties. T cells grafted with the combined CD28/CD3ζ signaling receptor secreted high amounts of IL-2 upon Ag binding without exogenous B7/CD28 costimulation, demonstrating that both MHC-independent cellular activation and CD28 costimulation for complete T cell activation can be delivered by one recombinant receptor molecule.

year	journal	country	edition	language
2001-11-21	Journal of immunology (Baltimore, Md. : 1950)

10.4049/jimmunol.167.11.6123 https://pubmed.ncbi.nlm.nih.gov/11714771