Discovery of an 8-Aza-5-thiaProstaglandin E1 Analog as a Highly Selective EP4 Receptor Agonist

Discovery of an 8-Aza-5-thiaProstaglandin E1 Analog as a Highly Selective EP4 Receptor Agonist

For the purpose of discovering an orally available EP4 subtype-selective agonist, a series of 8-aza prostaglandin E1 (PGE1) analogs were synthesized and evaluated for their affinity for PGE2 receptor subtypes. Additionally, the structure–activity relationships of these compounds were studied. Among...

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Veröffentlicht in:Chemical & Pharmaceutical Bulletin 2011/12/01, Vol.59(12), pp.1494-1508
Hauptverfasser: Kambe, Tohru, Maruyama, Toru, Naganawa, Atsushi, Asada, Masaki, Seki, Akiteru, Maruyama, Takayuki, Nakai, Hisao, Toda, Masaaki
Format: Artikel
Sprache:eng
Schlagworte:
agonist
Alprostadil - analogs & derivatives
Alprostadil - chemical synthesis
Alprostadil - chemistry
Alprostadil - metabolism
Alprostadil - pharmacology
EP4 receptor
Humans
Microsomes, Liver - metabolism
prostaglandin
Prostaglandins E, Synthetic - chemical synthesis
Prostaglandins E, Synthetic - chemistry
Prostaglandins E, Synthetic - metabolism
Prostaglandins E, Synthetic - pharmacology
Receptors, Prostaglandin E, EP2 Subtype - metabolism
Receptors, Prostaglandin E, EP4 Subtype - agonists
Receptors, Prostaglandin E, EP4 Subtype - metabolism
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Zusammenfassung:For the purpose of discovering an orally available EP4 subtype-selective agonist, a series of 8-aza prostaglandin E1 (PGE1) analogs were synthesized and evaluated for their affinity for PGE2 receptor subtypes. Additionally, the structure–activity relationships of these compounds were studied. Among the tested compounds, the 8-aza PGE1 analog 6 and 8-aza-5-thiaPGE1 analog 12 had highly potent EP4 receptor affinity, good functional activity, and excellent subtype-selectivity. Furthermore, these analogs demonstrated good stability in human liver microsomes. As a result, we concluded that these two series of 8-aza PGE1 analogs could be promising chemical leads for an orally available EP4 subtype-selective agonist.
ISSN:0009-2363
1347-5223
DOI:10.1248/cpb.59.1494