AGGREGATION OF PLATELETS INDUCED BY NOVEL SYNTHETIC SECOPROSTAGLANDINS
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概要
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Two series of 8-acetyl-12-hydroxyalkadienoic acids and 14-hydroxy-9-oxoalkadienoic acids which can be regarded as 11,12-and 8,12-secoprostaglandin E_2 were synthesized and evaluated for their biological properties. Key members of each series, 11,12-(8Ac-HAD) and 8,12-seco-11-norprostaglandin E_2 (14H-OAD), were found to induce platelet aggregation which were inhibited by preincubation of platelet rich plasma with prostaglandin I_2 but not inhibited by indomethacin. 8Ac-HAD produced dose-dependent potent contraction of rabbit aorta. Injection of 8Ac-HAD (1 mg/kg) into vein of rat induced sudden death of the animal. Both compounds were stable and platelet aggregating activity did not decrease at least for four hours at 0℃. Structure-activity relationship study of the series were carried out. Reduction of the acetyl carbonyl and methoxime formation of 8Ac-HAD lowered platelet aggregating acrivity, and 8-propionyl substituent and 12-deoxy derivative of 8Ac-HAD showed no activity. 12 (R)-Isomer and dl 12-methyl derivative of 8Ac-HAD retained the platelet aggregating activity. Modification of ω-chain did not cause any essential effect on the activity. Unlike 8Ac-HAD, several modification of 14H-OAD failed to maintain the aggregating activity.
- 公益社団法人日本薬学会の論文
著者
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OHTSU AKIRA
Teijin Institute for Biomedical Research
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TANAKA TOSHIO
Teijin Institute for Biomedical Research
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KAMIMOTO FUKUYOSHI
Teijin Institute for Biomedical Research
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HOSHINA KENJI
Teijin Institute for Biomedical Research
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KUROZUMI SEIZI
Teijin Institute for Biomedical Research
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NARUCHI TATSUYUKI
Teijin Institute for Biomedical Research
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OKAMIYA YOSHIAKI
Teijin Institute for Biomedical Research
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Naruchi Tatsuyuki
Teijin Institute For Bio-medical Research
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OKAMIYA Yoshiaki
Teijin Institute for Bio-medical Research, Hino
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