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Bioorganic and Medicinal Chemistry Letters 2013-Jun

Discovery of aryl ureas and aryl amides as potent and selective histamine H3 receptor antagonists for the treatment of obesity (part II).

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Il collegamento viene salvato negli appunti
Zhongli Gao
William J Hurst
Etienne Guillot
Werngard Czechtizky
Ulrike Lukasczyk
Raisa Nagorny
Marie-Pierre Pruniaux
Lothar Schwink
Juan Antonio Sanchez
Siegfried Stengelin

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Astratto

A novel series of histamine H3 receptor (H3R) antagonists was derived from an arylurea lead series (1) via bioisosteric replacement of the urea functionality by an amide linkage. The arylamide series was optimized through SAR studies by a broad variation of substituents in the left-hand side benzoyl residue (analogs 2a-2ag) or replacement of the benzoyl moiety by heteroarylcarbonyl residues (analogs 5a-5n). Compounds 2p and 2q were identified within the series as potent and selective H3R antagonists/inverse agonists with acceptable overall profile. Compound 2q was orally active in food intake inhibition in diet-induced obese (DIO) mice. Compound 2q represents a novel H3R antagonist template with improved in vitro potency and oral efficacy and has its merits as a new lead for further optimization.

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