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摘要:
Nanoliposome is a useful dosage form to increase solubility and absorption of simvastatin(SMV), and consequently improves its therapeutic effects. However, in vivo toxicity of SMV could also be elevated accompanied by the absorption enhancement, which is a decisive factor for the clinical application of SMV nanoliposome(SMV-Lipo), but has not been studied systematically and reported so far. In this study, organ toxicity of SMV-Lipo was evaluated in mice in the presence and absence of isoproterenol and compared to those of free SMV. Results demonstrated that compared to free SMV, the SMV-Lipo administrated at an equal dose of 25 mg/kg/d led to severe myocardiotoxicity, hepatotoxicity at baseline and more pronounced liver injury with elevation of alanine aminotransferase. In addition, muscular adverse effect was also observed in SMV-Lipo treated group but not in SMV group. Pharmacokinetic studies revealed that compared to free SMV, the SMV-Lipo administration significantly improved the plasma SMV concentration, and the oral bioavailability was 6.5 times of free SMV. Notably, when the dosage of free SMV increased to 50 mg/kg/d, yielding the comparable plasma concentration as SMV-Lipo given at 25 mg/kg/d, the myocardiotoxicity was observed in free SMV treated mice as well, which further confirmed that the enhanced absorption of SMV by the nanoliposomal formulation resulted in more severe myocardiotoxicity than the equal dose of free SMV.
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篇名 Simvastatin nanoliposome induces myocardial and hepatic toxicities due to its absorption enhancement in mice
来源期刊 亚洲药物制剂科学(英文) 学科 农学
关键词 SIMVASTATIN Nanoliposome Myocardiotoxicity MUSCULAR toxicity HEPATOTOXICITY
年,卷(期) 2020,(1) 所属期刊栏目
研究方向 页码范围 112-120
页数 9页 分类号 S43
字数 语种
DOI
五维指标
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研究主题发展历程
节点文献
SIMVASTATIN
Nanoliposome
Myocardiotoxicity
MUSCULAR
toxicity
HEPATOTOXICITY
研究起点
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研究分支
研究去脉
引文网络交叉学科
相关学者/机构
期刊影响力
亚洲药物制剂科学(英文)
双月刊
1818-0876
21-1608/R
中国沈阳市文化路103号107号信箱
8-624
出版文献量(篇)
70
总下载数(次)
0
总被引数(次)
0
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