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首页> 外文期刊>RSC Advances >Microbial transformation of diosgenin by Cunninghamella blakesleana AS 3.970 and potential inhibitory effects on P-glycoprotein of its metabolites
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Microbial transformation of diosgenin by Cunninghamella blakesleana AS 3.970 and potential inhibitory effects on P-glycoprotein of its metabolites

机译:Cunninghamella Blakesleana的微生物转化Duosgenin作为3.970的潜在抑制作用对其代谢物的p-糖蛋白

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摘要

Microbial transformation of diosgenin ((25R)-spirost-5-en-3 beta-ol) using Cunninghamella blakesleana AS 3.970, afforded eleven polyhydroxylated derivatives, including seven previously unreported steroids, such as 25(R)-spirost-5-en-3 beta,7 alpha,12 beta-triol (1), 25(R)-spirost-5-en-3 beta,7 alpha,12 beta,15 alpha,21-pentaol (3), 25(R)-spirost-5-en-3 beta,7 alpha,12 beta,18-tetraol (4), 25(R)-spirost-5-en-3 beta,7 alpha,12 beta,15 alpha-tetraol (5), 25(R)-spirost-5-en-3 beta,7 alpha,11 alpha,21-tetraol (6), 25(R)-spirost-5-en-3 beta,7 beta,15 alpha,21-tetraol (8), and 25(R)-spirost-5-en-3 beta,7 beta,12 beta,18-tetraol (10). The structures of metabolites 1-11 were elucidated by 1D-, 2D-NMR as well as HRESIMS techniques. Additionally, the biotransformation time-course of diosgenin by C. blakesleana AS 3.970 was presented. And the transformation pathway was also proposed on the basis of structural analyses and biotransformation time-courses. The P-glycoprotein (P-gp) inhibitory effects of these metabolites 1-11 were evaluated in a adriamycin resistant human breast adenocarcinoma cell line (MCF-7/ADR) at 20 mu M. And compounds 4 and 6 could increase the accumulation of adriamycin in MCF-7/ADR cells by approximately four times that of the control group, which suggested the significant potential P-glycoprotein inhibitory activities of 4 and 6. In silico docking analysis suggested that compound 4 had a similar P-gp recognition mechanism with verapamil (a classical inhibitor).
机译:使用Cunninghamella Blakesleana作为3.970的二氧((25r)-spirost-5-en-3β-oS)的微生物转化,得到11个多羟基化衍生物,包括七个先前未报告的类固醇,例如25(R)-Spirost-5-en- 3β,7α,12β-三醇(1),25(R)-Spirost-5-en-3β,7α,12β,15α,21-五戊烯(3),25(R)-Spirost -5-en-3β,7α,12β,18-四元(4),25(R)-spirost-5-en-3β,7α,12β,15α-四醇(5),25 (r)-pirost-5-en-3β,7α,11α,21-四醇(6),25(r)-spirost-5-en-3β,7β,15α,21-四醇( 8)和25(R)-Pirost-5-en-3β,7β,12β,18-四元(10)。由1D-,2D-NMR以及Hresims技术阐明代谢物1-11的结构。另外,提出了C.Blakesleana的Diosgenin的生物转化时间 - 作为3.970。并且还在结构分析和生物转化时间课程的基础上提出了转化途径。这些代谢物1-11的p-糖蛋白(p-gp)抑制作用在20 mu m的亚霉素抗性人乳腺腺癌细胞系(MCF-7 / ADR)中评估了这些代谢物1-11。化合物4和6可以增加积累在MCF-7 / ADR细胞中的亚霉素大约4倍的对照组,这表明在硅基对接分析中,4和6的显着潜在的p-糖蛋白抑制活性。该分析表明,化合物4具有类似的P-GP识别机制维拉帕米(古典抑制剂)。

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  • 来源
    《RSC Advances》 |2015年第95期|共9页
  • 作者

    Xu Min; Huo Xiao-Kui; Tian Xiang-Ge; Dong Pei-Pei; Wang Chao; Huang Shan-Shan; Zhang Bao-Jing; Zhang Hou-Li; Deng Sa; Ma Xiao-Chi;

  • 作者单位

    Dalian Med Univ Coll Pharm Dalian 116044 Peoples R China;

    Dalian Med Univ Coll Pharm Dalian 116044 Peoples R China;

    Dalian Med Univ Coll Pharm Dalian 116044 Peoples R China;

    Dalian Med Univ Acad Integrat Med Dalian 116044 Peoples R China;

    Dalian Med Univ Coll Pharm Dalian 116044 Peoples R China;

    Dalian Med Univ Coll Pharm Dalian 116044 Peoples R China;

    Dalian Med Univ Coll Pharm Dalian 116044 Peoples R China;

    Dalian Med Univ Coll Pharm Dalian 116044 Peoples R China;

    Dalian Med Univ Coll Pharm Dalian 116044 Peoples R China;

    Dalian Med Univ Coll Pharm Dalian 116044 Peoples R China;

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  • 正文语种 eng
  • 中图分类 化学;
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