Discovery and mechanism of action of small molecule inhibitors of ceramidases

Author:

Healey Robert D.,Saied Essa M.,Cong Xiaojing,Karsai Gergely,Gabellier Ludovic,Saint-Paul Julie,Nero Elise Del,Jeannot Sylvain,Drapeau Marion,Fontanel Simon,Maurel Damien,Basu Shibom,Leyrat Cedric,Bossis Guillaume,Bechara Cherine,Hornemann Thorsten,Arenz Christoph,Granier Sebastien

Abstract

AbstractSphingolipid metabolism is tightly controlled by enzymes to regulate essential processes such as energy utilisation and cell proliferation. The central metabolite is ceramide, a pro-apoptotic lipid catabolized by ceramidase enzymes to ultimately produce pro-proliferative sphingosine-1-phosphate. Human ceramidases can be soluble proteins (acid and neutral ceramidase) or integral membrane proteins (alkaline ceramidases). Increasing ceramide levels to increase apoptosis has shown efficacy as a cancer treatment using small molecules inhibiting a soluble ceramidase. Due to the transmembrane nature of alkaline ceramidases, no specific small molecule inhibitors have been reported. Here, we report novel fluorescent substrates (FRETceramides) of ceramidases that can be used to monitor enzyme activity in real-time. We use FRETceramides to discover the first drug-like inhibitors of alkaline ceramidase 3 (ACER3) which are active in cell-based assays. Biophysical characterization of enzyme:inhibitor interactions reveal a new paradigm for inhibition of lipid metabolising enzymes with non-lipidic small molecules.Table of contents summaryUse of synthetic fluorescent ceramide molecules allows the discovery of the first selective drug-like small molecule inhibitors for alkaline ceramidase 3, an intra-membrane enzyme involved in sphingolipid metabolism in health and disease.

Publisher

Cold Spring Harbor Laboratory

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