青藤碱N-取代衍生物的合成及抑制NF-κB转录活性作用
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烟台大学药学院,第二军医大学药学院有机化学教研室,第二军医大学药学院有机化学教研室,烟台大学药学院,烟台大学药学院

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上海市科委重点攻关项目(08431903003).


Synthesis of N-substituted sinomenine derivatives and its inhibitory effect against NF-κB transcriptional activity
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School of Pharmacy,Yantai University,Shandong,Department of Organic Chemistry,College of Pharmacy,Second Military Medical University,Department of Organic Chemistry,College of Pharmacy,Second Military Medical University,School of Pharmacy,Yantai University,Shandong,School of Pharmacy,Yantai University,Shandong

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Supported by Fund for Tackling Key Program of Shanghai Science and Technology Committee (08431903003).

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    摘要:

    目的 设计合成一类青藤碱衍生物,并研究其体外抗炎活性。方法 以青藤碱为原料,经脱N-甲基、亲核取代、经典的Click Reaction,共合成9个青藤碱衍生物,考察所得化合物体外对NF-κB转染的影响。结果 合成的目标化合物均为首次报道,并经1HNMR和LC-MS确证结构。所得化合物体外对NF-κB转染均具有一定的抑制作用,但活性较青藤碱有所下降。结论 N原子上引入较大基团或者长链可能会降低青藤碱的抗炎活性。

    Abstract:

    Objective To design and synthesize a series of sinomenine derivatives and to investigate their anti-inflammation activities in vitro. Methods Nine sinomenine derivatives were synthesized via demethylate of N atom, nucleophilic substitution and classical Click Reaction using sinomenine as the starting material. The target compounds were evaluated for their influence on NF-κB transcriptional activity in vitro. Results All the synthesized compounds were reported for the first time, and they were confirmed by 1HNMR and LC-MS. Biological studies showed that all the synthetic derivatives exhibited certain inhibitory effect against NF-κB transfection in vitro, but was weaker than that of sinomenine. Conclusion Replacing N-methyl with large group or long side chain on nitrogen atom may weaken the anti-inflammatory activity of sinomenine.

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  • 收稿日期:2014-10-11
  • 最后修改日期:2014-11-24
  • 录用日期:2015-01-12
  • 在线发布日期: 2015-04-17
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