物质信息
ID:73883
名称和标识
IUPAC标准名
(1S,3R,6S,8R,11S,12S,14R,15S,16R)-7,7,12,16-tetramethyl-6-(methylamino)-15-[(1S)-1-(methylamino)ethyl]pentacyclo[9.7.0.0^{1,3}.0^{3,8}.0^{12,16}]octadecan-14-ol
别名
BebuxineCyclovirobuxin D(Bebuxine)CyclovirobuxineCyclovirobuxine DNSC 91722
IUPAC传统名
(1S,3R,6S,8R,11S,12S,14R,15S,16R)-7,7,12,16-tetramethyl-6-(methylamino)-15-[(1S)-1-(methylamino)ethyl]pentacyclo[9.7.0.0^{1,3}.0^{3,8}.0^{12,16}]octadecan-14-ol
数据登录号
CAS号
化合物性质
安全信息
保存条件
-20°C
产品相关信息
成盐信息
Free Base
描述信息
Research Area: Cardiovascular Disease
Biological Activity:
Cyclovirobuxine D (bebuxine; Cyclovirobuxine) is an active compound extracted from Buxus microphylla, which has been used for treating acute myocardial ischemia. Cyclovirobuxine D (bebuxine; Cyclovirobuxine) significantly increased cardiomyocytes viability injured by oxidation or hypoxia. It significantly reduced the infarct size induced by ligating the coronary artery in rats, and the effect was almost abolished by glibenclamide, a blocker of ATP sensitive potassium channel, but it was not influenced by cyclooxygenase-2 inhibitor celecoxib or estrogen receptor antagonist tamoxifen. In addition, cyclovirobuxine D (bebuxine; Cyclovirobuxine) significantly protected rat aorta endothelial cells against hypoxia and enhanced nitric oxide (NO) release from endothelial cells, which was inhibited by nitric oxide synthase (NOS) inhibitor N-nitro-l-arginine methyl ester (L-NAME). Furthermore, cyclovirobuxine D (bebuxine; Cyclovirobuxine) significantly decreased the weight of venous thrombus in rats. [1][2]
Biological Activity:
Cyclovirobuxine D (bebuxine; Cyclovirobuxine) is an active compound extracted from Buxus microphylla, which has been used for treating acute myocardial ischemia. Cyclovirobuxine D (bebuxine; Cyclovirobuxine) significantly increased cardiomyocytes viability injured by oxidation or hypoxia. It significantly reduced the infarct size induced by ligating the coronary artery in rats, and the effect was almost abolished by glibenclamide, a blocker of ATP sensitive potassium channel, but it was not influenced by cyclooxygenase-2 inhibitor celecoxib or estrogen receptor antagonist tamoxifen. In addition, cyclovirobuxine D (bebuxine; Cyclovirobuxine) significantly protected rat aorta endothelial cells against hypoxia and enhanced nitric oxide (NO) release from endothelial cells, which was inhibited by nitric oxide synthase (NOS) inhibitor N-nitro-l-arginine methyl ester (L-NAME). Furthermore, cyclovirobuxine D (bebuxine; Cyclovirobuxine) significantly decreased the weight of venous thrombus in rats. [1][2]
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参考文献
• Grossini E et al. Life Sci. 1999;65(5):PL59-65.