Matrixglykane als multifunktionale Pathogenesefaktoren und therapeutische Zielstrukturen bei Tumorerkrankungen (GLYCANC)
Grunddaten zu diesem Projekt
Beschreibung
Cancer is a leading cause of mortality within the aging European population. Therapeutic targeting is hampered by the complexity of the disease, which includes not only molecular changes within the tumor cell itself, but also within its microenvironment. Tumor angiogenesis, tumor-stroma interactions, interactions with immune cells, with the extracellular matrix and cancer stem cell niches allow for malignant cell survival and promote metastasis, the leading cause for cancer-associated mortality. Proteoglycans (PGs) and glycosaminoglycans (GAGs) – structurally diverse carbohydrates of the extracellular matrix and cell surfaces - have emerged as novel biomarkers and molecular players both within tumor cells and their microenvironment, as they integrate signals from growth factors, chemokines and integrins, and cell-cell as well as matrix adhesion. Importantly, their expression is dysregulated in numerous tumor entities, and has been shown to modulate each of the hallmarks of cancer as defined by Hanahan and Weinberg (Cell 2011). We hypothesize that dysregulated function of PGs and GAGs simultaneously affects all molecular steps towards cancer metastasis as a general principle applicable to multiple tumor entities. Pharmacological modulation of their function thus emerges as an attractive multitargeted antitumoral approach which simultaneously acts at multiple levels of disease progression. Besides providing extensive knowledge transfer and training for researchers, the combined expertise of the GLYCANC consortium aims at performing a detailed structural analysis of PG and GAG glycans in disease using state-of-the art methodology, analysing their regulation via epigenetic mechanisms and microRNAs, and elucidating molecular mechanisms underlying aberrant PG and GAG function. GLYCANC will lead to a deeper understanding of glycan structures and glycan-dependent mechanisms promoting cancer progression, providing the basis for rational multitargeted anticancer approaches.
- EU H2020 - Marie Skłodowska-Curie Actions - Research and Innovation Staff Exchange (MSCA RISE)
Projektleitung der Universität Münster
| Götte, Martin |
Antragsteller*innen der Universität Münster
| Götte, Martin |
Projektbeteiligte Organisationen außerhalb der Universität Münster
- serend-ip GmbHDeutschland
- Fidia Farmaceutici SPAItalien
- Universität InsubriaItalien
- University of PatrasGriechenland
- Universität Reims Champagne-Ardenne (URCA)Frankreich
- National Centre of Scientific Research "Demokritos" (NCSR Demokritos)Griechenland
- Uppsala UniversitySchweden
- Semmelweis-Universität (SE)Ungarn
Publikationen der Universität Münster entstanden im Projekt
Viola M, Brüggemann K, Karousou E, Caon I, Caravà E, Vigetti D, Greve B, Stock C, De Luca G, Passi A, Götte M (2016) In: Glycoconjugate Journal, 2016. doi:10.1007/s10719-016-9735-6 Forschungsartikel (Zeitschrift) | Peer reviewed | Veröffentlicht | |
Ibrahim SA, Gadalla R, El-Ghonaimy EA, Samir O, Mohamed HT, Hassan H, Greve B, El-Shinawi M, Mohamed MM, Götte M (2017) In: Molecular Cancer, 16(1). doi:10.1186/s12943-017-0621-z Forschungsartikel (Zeitschrift) | Peer reviewed | Veröffentlicht | |
Piperigkou Z., Mohr B., Karamanos N., Götte M. (2016) In: Cell and Tissue Research, 365(3), 643-655. doi:10.1007/s00441-016-2452-4 Forschungsartikel (Zeitschrift) | Peer reviewed | Veröffentlicht | |
Karousou E., Misra S., Ghatak S., Dobra K., Götte M., Vigetti D., Passi A., Karamanos N., Skandalis S. (2016) In: Matrix Biology, 2016(null). doi:10.1016/j.matbio.2016.10.001 Forschungsartikel (Zeitschrift) | Peer reviewed | online first | |
Schwickert A., Weghake E., Brüggemann K., Engbers A., Brinkmann B., Kemper B., Seggewiß J., Stock C., Ebnet K., Kiesel L., Riethmüller C., Götte M. (2015) In: PloS one, 10(12). doi:10.1371/journal.pone.0143993 Forschungsartikel (Zeitschrift) | Peer reviewed | Veröffentlicht |
Preisverleihungen erhalten für Projekt
| Vortragspreis der Deutschen Gesellschaft für Senologie 2019 Verliehen von: Deutsche Gesellschaft für Senologie e.V. Verliehen an: Götte, Martin Bekannt gegeben am: 28.06.2019 | Verleihung erfolgte am: 28.06.2019 Art der Preisverleihung: Preis für beste Präsentation |
Vorträge zum Projekt
| MicroRNA miR–142–3p inhibits breast cancer cell invasiveness and stem cell properties by targeting integrin alpha V, KLF4 and multiple cytoskeletal elements Götte, Martin; (12.06.2016) 2nd Matrix Biology Europe Conference, Athen, Griechenland Art des Vortrags: wissenschaftlicher Vortrag | |
| Interplay of syndecan-1 and heparanase in cancer stem cell function Martin Götte (25.09.2015) 5th FEBS advanced lecture course 2015 - Matrix Pathobiology, Signaling and Molecular Targets, Rhodos, Griechenland Art des Vortrags: wissenschaftlicher Vortrag | |
| Role of Heparan Sulfate in Tumor-Initiating cells Götte; Martin (18.09.2015) 23rd Symposium on Glycosaminoglycans. Heparin centenary. Past, present and future perspectives , Villa Vigoni, Menaggio, Italien Art des Vortrags: wissenschaftlicher Vortrag | |
| Interplay of Syndecan-1 and Heparanase in Cancer Stem Cell Function Götte, Martin (23.08.2015) 9th International Conference on Proteoglycans and 10th Pan-Pacific Connective Tissue Societies Symposium, Seoul, Korea Art des Vortrags: wissenschaftlicher Vortrag |