Regulation of angiogenesis by targeting the melanoma microenvironment and its immune cells (B10#)

Subject Area Immunology

Term from 2015 to 2021

Project identifier Deutsche Forschungsgemeinschaft (DFG) - Project number 68647618

Project Description

We identified how highly efficient anti-tumor immune responses can be initiated by specific activation of melanoma-resident mast cells (MC). Tumor-infiltrating effector T cells (TILs) were recruited by MC-derived CXCL10 and preliminary data indicate that inhibition of angiogenesis is potently participating in this efficient tumor immune control. Thus, the inhibition of angiogenesis as part of tumor immune therapy will be mechanistically investigated with a focus on MC and TILs. Importantly, by support of the CRC tumor control, T-cell recruitment, and inhibition of angiogenesis in mice and humans will be imaged allowing the appropriate adjustments to further optimize treatment of melanoma.

DFG Programme Collaborative Research Centres

Subproject of SFB 824: Imaging for Selection, Monitoring and Individualisation of Cancer Therapies

Applicant Institution Technische Universität München (TUM)

Project Head Professor Dr. Tilo Biedermann

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Regulation of angiogenesis by targeting the melanoma microenvironment and its immune cells (B10#)

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Servicenavigation

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Regulation of angiogenesis by targeting the melanoma microenvironment and its immune cells (B10#)

Additional Information

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