The Evolution of T-cell Dysfunction in AML – Tailored Antibody-based Immunotherapy to Increase Response Rate and Overcome Innate and Adaptive Resistance

Applicants Professor Dr. Karl-Peter Hopfner; Professorin Dr. Marion Subklewe

Subject Area Hematology, Oncology
Biochemistry
Immunology

Term from 2020 to 2023

Project identifier Deutsche Forschungsgemeinschaft (DFG) - Project number 451580403

Project Description

Treatment of AML by allogeneic stem cell transplantation is mediated by T cells but is hampered by a high mortality rate. We find that T-cell function is modulated through progressively evolving changes in phenotype and function of AML. Our goal is to unravel changes in T-cell responses and develop multi-specific anti¬body derivatives (msADs), tailored to interfere with immune checkpoint molecules in specific geno- and phenotype of AML subtypes.

DFG Programme Research Grants

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The Evolution of T-cell Dysfunction in AML – Tailored Antibody-based Immunotherapy to Increase Response Rate and Overcome Innate and Adaptive Resistance

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Servicenavigation

Hauptnavigation

The Evolution of T-cell Dysfunction in AML – Tailored Antibody-based Immunotherapy to Increase Response Rate and Overcome Innate and Adaptive Resistance

Additional Information

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