Sphingolipid- and Matrix –mediated Signalling pathways in chronic inflamation and fibrosis of the kidney (B02)

Subject Area Pharmacology

Term since 2013

Project identifier Deutsche Forschungsgemeinschaft (DFG) - Project number 204083920

Project Description

This project aims at investigating the therapeutic potential of specific inhibitors of S1PR5, the Spns2 transporter and of a novel S1PR1 G protein-biased agonist for an antifibrotic effect in kidney injury models. Mechanistically, the decreased degradation of antifibrotic Smad7 due to sphingosin-mediated reduction of ubiquitin ligases will be elucidated. Further experiments will particularly address the impact of specific chain-lengths of S1P and the crosstalk of S1P and the proteoglycan biglycan in renal inflammation, resolution and fibrosis.

DFG Programme Collaborative Research Centres

Subproject of SFB 1039: Signalling by Fatty Acid Derivatives and Sphingolipids in Health and Disease

Applicant Institution Goethe-Universität Frankfurt am Main

Project Heads Professor Dr. Josef M. Pfeilschifter; Professorin Dr. Liliana Schaefer

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Hauptnavigation

Sphingolipid- and Matrix –mediated Signalling pathways in chronic inflamation and fibrosis of the kidney (B02)

Additional Information

Servicenavigation

Hauptnavigation

Sphingolipid- and Matrix –mediated Signalling pathways in chronic inflamation and fibrosis of the kidney (B02)

Additional Information

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