Studies on the Mechanism of Action of the Gastric H+, K+-ATPase Inhibitor SPI-447

Yasuhiro Tsukimi; Toshihisa Ushiro; Takashi Yamazaki; Harumi Ishikawa; Jyoji Hirase; Mitsuhiro Narita; Toshiki Nishigaito; Kimiko Banno; Toshio Ichihara; Hironori Tanaka

doi:10.1254/jjp.82.21

Full Papers

Studies on the Mechanism of Action of the Gastric H⁺, K⁺-ATPase Inhibitor SPI-447

Yasuhiro Tsukimi, Toshihisa Ushiro, Takashi Yamazaki, Harumi Ishikawa, Jyoji Hirase, Mitsuhiro Narita, Toshiki Nishigaito, Kimiko Banno, Toshio Ichihara, Hironori Tanaka

Author information

Yasuhiro Tsukimi
Department of New Drug Research Laboratories,Technical Headquarters,Shinnippon Pharmaceutical,Inc.,370 Mita,Kishiwada 596-0808,Japan
Toshihisa Ushiro
Department of New Drug Research Laboratories,Technical Headquarters,Shinnippon Pharmaceutical,Inc.,370 Mita,Kishiwada 596-0808,Japan
Takashi Yamazaki
Department of New Drug Research Laboratories,Technical Headquarters,Shinnippon Pharmaceutical,Inc.,370 Mita,Kishiwada 596-0808,Japan
Harumi Ishikawa
Department of New Drug Research Laboratories,Technical Headquarters,Shinnippon Pharmaceutical,Inc.,370 Mita,Kishiwada 596-0808,Japan
Jyoji Hirase
Department of New Drug Research Laboratories,Technical Headquarters,Shinnippon Pharmaceutical,Inc.,370 Mita,Kishiwada 596-0808,Japan
Mitsuhiro Narita
Department of New Drug Research Laboratories,Technical Headquarters,Shinnippon Pharmaceutical,Inc.,370 Mita,Kishiwada 596-0808,Japan
Toshiki Nishigaito
Department of New Drug Research Laboratories,Technical Headquarters,Shinnippon Pharmaceutical,Inc.,370 Mita,Kishiwada 596-0808,Japan
Kimiko Banno
Department of New Drug Research Laboratories,Technical Headquarters,Shinnippon Pharmaceutical,Inc.,370 Mita,Kishiwada 596-0808,Japan
Toshio Ichihara
Department of New Drug Research Laboratories,Technical Headquarters,Shinnippon Pharmaceutical,Inc.,370 Mita,Kishiwada 596-0808,Japan
Hironori Tanaka
Department of New Drug Research Laboratories,Technical Headquarters,Shinnippon Pharmaceutical,Inc.,370 Mita,Kishiwada 596-0808,Japan

Keywords: H⁺, K⁺-ATPase inhibitor, Anti-ulcer drug, SPI-447, Omeprazole, SCH28080

JOURNAL FREE ACCESS

2000 Volume 82 Issue 1 Pages 21-28

DOI https://doi.org/10.1254/jjp.82.21

Details

Abstract

3−Amino−5−methyl−2(2−methyl−3−thienyl)−imidazo[1, 2−a]thieno[3, 2−c]pyridine, SPI−447, is a potent gastric H⁺, K⁺−ATPase inhibitor, but a detailed mechanism of the inhibition is unknown.This study was designed to investigate the mechanism by which SPI−447 inhibits gastric H⁺, K⁺−ATPase.For this purpose, the inhibitory action of SPI−447 on gastric H⁺, K⁺−ATPase from porcine gastric mucosa was compared with that of omeprazole(an irreversible inhibitor)and SCH28080(a reversible inhibitor).All compounds produced dose−dependent inhibition of gastric H⁺, K⁺−ATPase, and the inhibitory intensities were increased under acidic conditions.The anti−H⁺, K⁺−ATPase actions of SPI−447 and SCH28080 were attenuated by dilution, but not influenced by glutathione pretreatment.In contrast, that of omeprazole was not influenced by dilution, but was suppressed by glutathione pretreatment.KCl addition reversed the inhibition of H⁺, K⁺−ATPase−mediated H⁺−transport by SPI−447 and SCH28080, but had no effect on that by omeprazole.The anti−gastric H⁺, K⁺−ATPase action of SPI−447 was additive with that of SCH28080.SPI−447 and SCH28080 had no effect on Na⁺, K⁺−ATPase activity.These findings indicated that the inhibitory mechanism of SPI−447 on gastric H⁺, K⁺−ATPase was similar to that of SCH28080, but different from that of omeprazole;i.e., 1)reversible, 2)SH−group independent, 3)K⁺−competitive, and 4)highly specific against gastric H⁺, K⁺−ATPase.

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