Project Details
Projekt
Molecular T cell immunotherapy and inhibition of tumor immune escape mechanisms (06)
Subject Area
Immunology
Term
since 2018
Project identifier
Deutsche Forschungsgemeinschaft (DFG) - Project number 318346496
We have demonstrated that (i) the tumour suppressor p53-encoded 133p53 isoform functions as a novel enhancer of cellular resilience of antitumoural TCR-engineered T cells and (ii) arginase 1 inhibition unleashes a highly potent T cell stimulatory activity within the secretome of human granulocytes. We now want to fully characterize the hyperactivated T cells, identify the molecular correlate of the hyperstimulatory activity and analyse its therapeutic potential in conjunction with 33p53 T cell modification. The tumour microenvironment will be studied in depth and our novel strategy will be extended to other tumour and infectious disease models within the CRC.
DFG Programme
Collaborative Research Centres
Subproject of
SFB 1292:
Targeting convergent mechanisms of inefficient immunity in tumors and chronic infections
Applicant Institution
Johannes Gutenberg-Universität Mainz
Project Heads
Professor Dr. Markus Munder; Professor Dr. Matthias Theobald
