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De Novo Conception of Small Molecule Modulators Based on Endogenous Peptide Ligands: Pyrrolodiazepin-2-one gamma-Turn Mimics That Differentially Modulate Urotensin II Receptor-Mediated Vasoconstriction ex Vivo

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Dufour-Gallant, Julien; Chatenet, David et Lubell, William D (2015). De Novo Conception of Small Molecule Modulators Based on Endogenous Peptide Ligands: Pyrrolodiazepin-2-one gamma-Turn Mimics That Differentially Modulate Urotensin II Receptor-Mediated Vasoconstriction ex Vivo Journal of Medicinal Chemistry , vol. 58 , nº 11. pp. 4624-37. DOI: 10.1021/acs.jmedchem.5b00162.

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Résumé

A proof-of-concept library of pyrrolodiazepinone small molecules was designed based on the Bip-Lys-Tyr motif found in a recently described modulator of the urotensinergic system. Solid-phase synthesis provided 13 analogues, which were tested for their ability to modulate selectively and differentially the potency (EC50) and efficacy (Emax) of hUII and URP ex vivo in a rat aortic ring bioassay. Notably, at 14 muM, pyrrolodiazepinone R-4a inhibited completely hUII-induced contractions and increased URP-associated vasoconstriction. Pyrrolodiazepinone R-4a represents, to the best of our knowledge, a first-in-class small molecule that exerts a probe-dependent effect on hUII and URP biological activities and proves that UT modulators of the urotensin II receptor (UT) can be rationally designed. The importance of the UT system in the pathogenesis and progression of cardiovascular diseases highlights the utility of pyrrolodiazepinones such as R-4a, which exhibit promising potential as tools for differentiating the respective roles, signaling pathways, and phenotypic outcomes of UII and URP in the UT system.

Type de document: Article
Mots-clés libres: PULMONARY ARTERIAL-HYPERTENSION; BETA-D-GLUCOSE; DRUG DISCOVERY; PHARMACOLOGICAL CHARACTERIZATION; CONFORMATIONAL-ANALYSIS; COLLAGEN-SYNTHESIS; HEART-FAILURE; BINDING MODE; RAT AORTA; ANTAGONISTS
Centre: Centre INRS-Institut Armand Frappier
Date de dépôt: 16 mai 2017 20:41
Dernière modification: 16 mai 2017 20:41
URI: https://espace.inrs.ca/id/eprint/3179

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