
Bioorganic and Medicinal Chemistry p. 1695 - 1714 (1997)
Update date:2022-08-03
Topics:
Hagishita, Sanji
Murakami, Yasushi
Seno, Kaoru
Kamata, Susumu
Haga, Nobuhiro
Konoike, Toshiro
Kanda, Yasuhiko
Kiyama, Ryuichi
Shiota, Takeshi
Ishihara, Yasunobu
Ishikawa, Michio
Shimamura, Mayumi
Abe, Koji
Yoshimura, Koji
A novel series of CCK-B/gastrin receptor antagonists - ureidomethylcarbamoylphenylketone derivatives - were designed, synthesized, and evaluated for activity. Structure-activity relationship studies revealed the importance of a carboxylic acid at substituent R2 and a tert-butoxycarbonyl group at R1 in structure A. Compound 7a (S-0509) showed remarkable affinity for the CCK-B/gastrin receptor and a subtype selectivity profile in vitro. Administration (id) of 7a led to excellent inhibition of gastric acid secretion induced by pentagastrin in anesthetized rats with an ED50 value of 0.014 mg/kg. Furthermore, 7a proved to have poor blood-brain permeability by its small effect on enhancement of morphine analgesia. Thus, S-0509 has an increase in selectivity for the peripheral effects of gastrin antagonism from the central effects of CCK-B antagonism.
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Doi:10.1021/ja01024a046
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