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首页> 外文期刊>Chemical and Pharmaceutical Bulletin >C-Homomorphinan Derivatives as Lead Compounds to Obtain Safer and More Clinically Useful Analgesics
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C-Homomorphinan Derivatives as Lead Compounds to Obtain Safer and More Clinically Useful Analgesics

机译:作为铅化合物的C-同源物衍生物获得更安全,更临床上有用的镇痛药

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摘要

Buprenorphine shows strong analgesic effects on moderate to severe pain. Although buprenorphine can be used more safely than other opioid analgesics, it has room for improvement in clinical utility. Investigation of compounds structurally related to buprenorphine should be an approach to obtain novel analgesics with safer and improved profiles compared to buprenorphine. In the course of our previous studies, we observed that derivatives obtained by cyclizing C-homomorphinans were structurally related to buprenorphine. Hence, we synthesized cyclized C-homomorphinan derivatives with various oxygen functionalities on the side chains and evaluated their in vitro pharmacological profiles for the opioid receptors. Among the tested compounds, methyl ketone 2a with an N-methyl group showed full agonistic activities for the mu and the delta receptors and partial agonistic activity for the kappa receptor. These properties were similar to those of norbuprenorphine, a major metabolite of buprenorphine, which reportedly contributes to the antinociceptive effect of buprenorphine. From these results, we concluded that cyclized C-homomorphinan would be a possible lead compound to obtain novel analgesics with buprenorphine-like properties.
机译:丁甲啡对中度至严重疼痛表现出强烈的镇痛作用。虽然丁丙诺啡可以比其他阿片类镇痛药更安全地使用,但它有临床效用的改善空间。与丁丙诺啡有关的化合物的研究应该是与Buprenorphine相比具有更安全和改善的曲线的新镇痛药的方法。在我们以前的研究过程中,我们观察到通过旋滑C-同源体获得的衍生物与丁丙诺啡有关。因此,我们在侧链上合成了环状的C-同源衍生物,并在侧链上具有各种氧官能团,并评估其体外药理学谱的阿片类药物。在测试的化合物中,用N-甲基的甲基酮2a显示穆和δ受体的全激动活性,以及​​κ受体的部分激动活性。这些性质与Norbuprenorphine的性质类似,丁丙诺啡的主要代谢物,据报道促进了丁丙诺啡的抗伤害作用。从这些结果来看,我们得出结论,环化的C-同源鱼是一种可能的铅化合物,以获得具有丁丙诺啡样特性的新型镇痛药。

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  • 来源
    《Chemical and Pharmaceutical Bulletin》 |2017年第10期|共10页
  • 作者

    Ishikawa Kyoko; Karaki Fumika; Tayama Kaoru; Higashi Eika; Hirayama Shigeto; Itoh Kennosuke; Fujii Hideaki;

  • 作者单位

    Kitasato Univ Sch Pharm Med Chem Lab Minato Ku 5-9-1 Shirokane Tokyo 1088641 Japan;

    Kitasato Univ Sch Pharm Med Chem Lab Minato Ku 5-9-1 Shirokane Tokyo 1088641 Japan;

    Kitasato Univ Sch Pharm Med Chem Lab Minato Ku 5-9-1 Shirokane Tokyo 1088641 Japan;

    Kitasato Univ Sch Pharm Med Chem Lab Minato Ku 5-9-1 Shirokane Tokyo 1088641 Japan;

    Kitasato Univ Sch Pharm Med Chem Lab Minato Ku 5-9-1 Shirokane Tokyo 1088641 Japan;

    Kitasato Univ Sch Pharm Med Chem Lab Minato Ku 5-9-1 Shirokane Tokyo 1088641 Japan;

    Kitasato Univ Sch Pharm Med Chem Lab Minato Ku 5-9-1 Shirokane Tokyo 1088641 Japan;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 药学;化学;
  • 关键词

    opioid; C-homomorphinan; buprenorphine;

    机译:阿片类化合物;C-同源物;Buprenorphine;

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