Discovery of Novel Benzoxazinones as Potent and Orally Active Long Chain Fatty Acid Elongase 6 Inhibitors

Discovery of Novel Benzoxazinones as Potent and Orally Active Long Chain Fatty Acid Elongase 6 Inhibitors

A series of benzoxazinones was synthesized and evaluated as novel long chain fatty acid elongase 6 (ELOVL6) inhibitors. Exploration of the SAR of the UHTS lead 1a led to the identification of (S)-1y that possesses a unique chiral quarternary center and a pyrazole ring as critical pharmacophore eleme...

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Veröffentlicht in:Journal of medicinal chemistry 2009-11, Vol.52 (22), p.7289-7300
Hauptverfasser: Mizutani, Takashi, Ishikawa, Shiho, Nagase, Tsuyoshi, Takahashi, Hidekazu, Fujimura, Takashi, Sasaki, Takahide, Nagumo, Akira, Shimamura, Ken, Miyamoto, Yasuhisa, Kitazawa, Hidefumi, Kanesaka, Maki, Yoshimoto, Ryo, Aragane, Katsumi, Tokita, Shigeru, Sato, Nagaaki
Format: Artikel
Sprache:eng
Schlagworte:
Acetyltransferases - antagonists & inhibitors
Acetyltransferases - metabolism
Administration, Oral
Animals
Benzoxazines - administration & dosage
Benzoxazines - chemical synthesis
Benzoxazines - chemistry
Benzoxazines - pharmacology
Biological and medical sciences
Cell Line, Tumor
Drug Discovery
Enzyme Inhibitors - administration & dosage
Enzyme Inhibitors - chemical synthesis
Enzyme Inhibitors - chemistry
Enzyme Inhibitors - pharmacology
Fatty Acids - blood
Fatty Acids - metabolism
General and cellular metabolism. Vitamins
Humans
Liver - drug effects
Liver - metabolism
Male
Medical sciences
Mice
Pharmacology. Drug treatments
Structure-Activity Relationship
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Beschreibung
Zusammenfassung:A series of benzoxazinones was synthesized and evaluated as novel long chain fatty acid elongase 6 (ELOVL6) inhibitors. Exploration of the SAR of the UHTS lead 1a led to the identification of (S)-1y that possesses a unique chiral quarternary center and a pyrazole ring as critical pharmacophore elements. Compound (S)-1y showed potent and selective inhibitory activity toward human ELOVL6 while displaying potent inhibitory activity toward both mouse ELOVL3 and 6 enzymes. Compound (S)-1y showed acceptable pharmacokinetic profiles after oral dosing in mice. Furthermore, (S)-1y significantly suppressed the elongation of target fatty acids in mouse liver at 30 mg/kg oral dosing.
ISSN:0022-2623
1520-4804
DOI:10.1021/jm900915x