Design, synthesis and identification of novel benzimidazole derivatives as highly potent NPY Y5 receptor antagonists with attractive in vitro ADME profiles

Design, synthesis and identification of novel benzimidazole derivatives as highly potent NPY Y5 receptor antagonists with attractive in vitro ADME profiles

Optimization of our HTS hit 1, mainly focused on modification at the C-2 position of the benzimidazole core, is described. Elimination of the flexible and metabolically labile –S-CH2– part and utilization of less lipophilic pyridone substructure led to identification of novel NPY Y5 receptor antagon...

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Veröffentlicht in:Bioorganic & medicinal chemistry letters 2012-09, Vol.22 (17), p.5498-5502
Hauptverfasser: Tamura, Yuusuke, Omori, Naoki, Kouyama, Naoki, Nishiura, Yuji, Hayashi, Kyouhei, Watanabe, Kana, Tanaka, Yukari, Chiba, Takeshi, Yukioka, Hideo, Sato, Hiroki, Okuno, Takayuki
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Antagonists
Benzimidazole
Benzimidazoles - chemical synthesis
Benzimidazoles - chemistry
Benzimidazoles - metabolism
Benzimidazoles - pharmacology
binding capacity
Biological and medical sciences
chemistry
Cytochrome P-450 Enzyme Inhibitors
Cytochrome P-450 Enzyme System - metabolism
Drug Design
Humans
Lipophilic
Medical sciences
Mice
Microsomes, Liver - metabolism
Neuropeptide Y5 receptors
NPY Y5 receptor antagonist
Obesity
Obesity - drug therapy
Pharmacology. Drug treatments
Pyridone
Pyridones - chemical synthesis
Pyridones - chemistry
Pyridones - metabolism
Pyridones - pharmacology
Rats
Receptors, Neuropeptide Y - antagonists & inhibitors
Receptors, Neuropeptide Y - metabolism
Solubility
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Zusammenfassung:Optimization of our HTS hit 1, mainly focused on modification at the C-2 position of the benzimidazole core, is described. Elimination of the flexible and metabolically labile –S-CH2– part and utilization of less lipophilic pyridone substructure led to identification of novel NPY Y5 receptor antagonists 6, which have low to sub-nanomolar Y5 receptor binding affinity with improved CYP450 inhibition profiles, good solubilities and high metabolic stabilities.
ISSN:0960-894X
1464-3405
DOI:10.1016/j.bmcl.2012.07.020