Research Group

Immune Modulation in Cancer

Dr. Martina Seiffert

Our research group investigates tumor immunology and the microenvironment of non-Hodgkin B-cell lymphomas as well as brain metastases from breast and lung cancer, focusing on cancer-induced immunosuppression and T-cell exhaustion to develop novel immunotherapies in patient-based models.

Our research

We are interested in tumor immunology and the microenvironment in non-Hodgkin's B-cell lymphoma and brain metastases from breast and lung cancer. In particular, we investigate mechanisms of cancer-induced immunosuppression and T-cell exhaustion as pathological factors in cancer. Our aim is to identify mediators and molecular mechanisms of interactions between cancer cells and their environment, focusing on immune cells of the myeloid and lymphoid lineages. We use our findings to develop and test novel immunotherapy approaches in patient-based coculture models and genetic mouse lines.

The complex cellular and molecular composition of tumors is essential for their pathobiology. We have previously identified molecular mechanisms and candidate molecules responsible for cancer-induced remodeling of the microenvironment and immune system.

Our current work focuses on an in-depth characterization of immune and stromal cells in B-cell lymphomas and brain metastases, with the aim of elucidating novel pro-tumorigenic and immunosuppressive mechanisms, as well as identifying candidate genes and signaling pathways for the development of new therapeutic approaches. This also includes the definition of new prognostic or predictive biomarkers and the identification of mechanisms of therapy resistance. We are particularly interested in cancer-associated T cell exhaustion, the immunosuppressive function of myeloid cells, and the mediators responsible for these two phenotypes. Ongoing projects focus on interleukin-10 (IL-10), interleukin-4-induced-1 (IL4I1) and galectin-9.

We use single cell transcriptome analysis, spectral flow cytometry and proteomic analysis to study primary tumor tissue and blood cells, multiplex immunofluorescence staining and in situ transcript quantification of tissue sections to spatially map the tumor microenvironment, as well as functional assays and treatment studies in vitro and in mouse models to validate the relevance of identified candidate genes and pathways. Our preclinical therapy studies also include the optimization of the treatment of CLL and DLBCL with CAR T-cell products and bispecific antibodies.

To this end, we cooperate with academic and industry partners and are in close contact with our colleagues in the clinic.

Team

18 Employees

  • Dr. Martina Seiffert

    Group leader

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  • Dr. Nicolas Aubert

    Postdoc

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  • Yuliia Borysovych

    PhD student

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  • Hannah Briesch

    PhD student

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  • Covadonga Castellanos Gonzalez

    PhD student

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  • Dr. Celia Dobano-Lopez

    Postdoc

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  • Alessia Flörchinger

    PhD student

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  • Dr. Mohana Krishna Gopisetty

    Postdoc

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  • Julia Hartmann

    PhD student

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  • Lena Jassowicz

    Postdoc

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  • Sibylle Ohl

    Technical assistant

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  • Liesa-Marie Pilger

    PhD student

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  • Changgyun Park

    Postdoc

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  • Lucie Rospape

    Internship

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  • Dr. Philipp Rößner

    Scientist

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  • Angelika Schermer

    Technical assistant

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  • Dr. Mathieu Virazels

    Postdoc

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  • Jan Schadendorf

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Selected publications

2025 - Nat Comms, accepted on 15.01.2025

Longitudinal omics data and preclinical treatment suggest the proteasome inhibitor carfilzomib as therapy for ibrutinib-resistant CLL.

2024 - Blood 2024 Aug 1;144(5):510-524
2024 - Blood 2024 Aug 15;144(7):784-789
2021 - Immunity, 54(12): 2825-2841
2020 - Cell 2020 Sep 3;182(5):1252-1270

Reviews

2024 - Hematol, 61(3): 194-200
2020 - Leukemia, 34(8): 2012-2024
2017 - Mol Immunol, 110: 77-87

Get in touch with us

Dr. Martina Seiffert
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