In depth investigation of the molecular signaling mechanisms and cellular function of midkine, neuropilin-2 and sFLT1 in conjunctival and uveal melanoma (C03)

Subject Area Ophthalmology

Term since 2024

Project identifier Deutsche Forschungsgemeinschaft (DFG) - Project number 501530074

Project Description

To develop effective therapies for metastatic ocular melanoma, it is of utmost importance to understand the underlying cellular and molecular mechanisms behind metastasis in ocular melanoma. In our previous studies, we were able to identify that lymphangiogenesis is a decisive risk factor for metastatic spread in ocular melanoma. In the present project, the characterization of cellular functions and molecular signaling pathways involving the key drivers of ocular tumor metastasis, Midkine, NRP2 and sFLT1, are studied with the long-term goal to translate our findings into clinically used (neo)adjuvant, antilymphatic therapeutic strategies for ocular melanoma patients.

DFG Programme Collaborative Research Centres

Subproject of SFB 1607: Towards immunomodulatory and anti(lymph)angiogenic therapies for age-related blinding eye diseases

Applicant Institution Universität zu Köln

Project Heads Dr. Jacobus J. Bosch; Professor Dr. Ludwig M. Heindl

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In depth investigation of the molecular signaling mechanisms and cellular function of midkine, neuropilin-2 and sFLT1 in conjunctival and uveal melanoma (C03)

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Servicenavigation

Hauptnavigation

In depth investigation of the molecular signaling mechanisms and cellular function of midkine, neuropilin-2 and sFLT1 in conjunctival and uveal melanoma (C03)

Additional Information

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