| Literature DB >> 34668624 |
Robert D Healey1, Essa M Saied2,3, Xiaojing Cong1, Gergely Karsai4, Ludovic Gabellier5, Julie Saint-Paul1, Elise Del Nero1, Sylvain Jeannot1, Marion Drapeau1, Simon Fontanel1, Damien Maurel1, Shibom Basu6, Cedric Leyrat1, Jérôme Golebiowski7,8, Guillaume Bossis5, Cherine Bechara1,9, Thorsten Hornemann4, Christoph Arenz2, Sebastien Granier1.
Abstract
Sphingolipid metabolism is tightly controlled by enzymes to regulate essential processes in human physiology. The central metabolite is ceramide, a pro-apoptotic lipid catabolized by ceramidase enzymes to produce pro-proliferative sphingosine-1-phosphate. Alkaline ceramidases are transmembrane enzymes that recently attracted attention for drug development in fatty liver diseases. However, due to their hydrophobic nature, no specific small molecule inhibitors have been reported. We present the discovery and mechanism of action of the first drug-like inhibitors of alkaline ceramidase 3 (ACER3). In particular, we chemically engineered novel fluorescent ceramide substrates enabling screening of large compound libraries and characterized enzyme:inhibitor interactions using mass spectrometry and MD simulations. In addition to revealing a new paradigm for inhibition of lipid metabolising enzymes with non-lipidic small molecules, our data lay the ground for targeting ACER3 in drug discovery efforts.Entities:
Keywords: FRET screening assay; ceramidase; intramembrane enzyme inhibition; lipid metabolism; structural dynamics
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Year: 2021 PMID: 34668624 DOI: 10.1002/anie.202109967
Source DB: PubMed Journal: Angew Chem Int Ed Engl ISSN: 1433-7851 Impact factor: 15.336