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Discovery of New Nanomolar Selective IRAP Inhibitors

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He, Ben | Karroum, Nour Bou | Gealageas, Ronan | Mauvais, François-Xavier | Warenghem, Sandrine | Roignant, Matthieu | Kraupner, Nicolas | Lam, Bao Vy | Azaroual, Nathalie | Ultré, Vincent | Rech, Alexandre | Lesire, Laetitia | Couturier, Cyril | Leroux, Florence | van Endert, Peter | Deprez, Benoit | Deprez-Poulain, Rebecca

Edité par CCSD ; American Chemical Society -

International audience. Among the M1 family of oxytocinase aminopeptidases, insulin-regulated aminopeptidase IRAP, is an emerging drug target implicated in various biological pathways and particularly in MHC-I antigen presentation through amino-terminal trimming of exogenous cross-presented peptides. A few series of inhibitors inspired either by angiotensin IV, one of IRAP substrates, or by bestatin a pan aminopeptidase inhibitor, have been disclosed. However, the variety and number of chemotypes remains relatively limited. Here we disclose the design and optimization of a series of hydroxamic acids IRAP inhibitors bearing a 5-substituted indole. Docking studies of the best compound 43 (BDM_92499), a single-digit nanomolar and selective inhibitor of IRAP, suggest an original binding mode and highlight the substituent on the indole and a primary amide as groups driving selectivity. Several inhibitors in the series displayed IRAP-dependent inhibition of antigen cross-presentation. These results pave the way to the development of novel therapeutic agents targeting IRAP.

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