Synthesis and evaluation of new arylsulfonamidomethylcyclohexyl derivatives as human neuropeptide Y Y5 receptor antagonists for the treatment of obesity.

Authors :: Moreno A
Pérez S
Galiano S
Juanenea L
Erviti O
Frígola C
Aldana I
Monge A
Source :: European journal of medicinal chemistry [Eur J Med Chem] 2004 Jan; Vol. 39 (1), pp. 49-58.
Publication Year :: 2004
Abstract: NPY is the most potent orexigenic peptide identified up to now. Stimulation of food intake is measured by the Y(1) and Y(5) receptor subtypes. In this study, the synthesis and evaluation of new arylsulfonamidomethylcyclohexyl derivatives are described as potential selective antagonists of the human NPY Y(5) receptor. The SAR of these series was examined and the amide derivatives were the compounds that showed the best activities. trans-N-(4-[(Quinolin-3-yl)aminocarbonyl]cyclohexylmethyl)-2,4-dichlorobenzenesulfonamide (42) bound to the human neuropeptide Y Y(5) receptor with a 2 nM IC(50).

Subjects :: Animals
Binding, Competitive drug effects
Cell Line
Drug Evaluation, Preclinical
Humans
Molecular Structure
Obesity drug therapy
Structure-Activity Relationship
Anti-Obesity Agents pharmacology
Cyclohexanes chemical synthesis
Cyclohexanes pharmacology
Receptors, Neuropeptide Y antagonists & inhibitors
Sulfonamides chemical synthesis
Sulfonamides pharmacology

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