京尼平
细胞毒性
栀子花
化学
立体化学
癌细胞系
硅烷化
硅醚
细胞毒性T细胞
组合化学
癌细胞
生物化学
癌症
生物
体外
壳聚糖
医学
病理
催化作用
替代医学
遗传学
作者
Patamawadee Silalai,Uthaiwan Sirion,Pawinee Piyachaturawat,Arthit Chairoungdua,Kanoknetr Suksen,Rungnapha Saeeng
标识
DOI:10.1002/slct.202001908
摘要
Abstract Genipin 1 , derived from geniposide present in the fruit of Gardenia jasminoides Ellis has been reported to show diverse pharmacological activity. In this work, a new series of genipin‐triazole analogues was designed and synthesized yielding high yields from naturally genipin and their cytotoxicity evaluated against six cancer cell lines. Twenty‐seven analogues were obtained using a convenient four‐step reaction methods. Six analogues showed higher cytotoxic activity than the original genipin and benzylether‐triazolegenipin 5 j exhibited the strongest activity against P‐388 and A‐549 cancer cell lines with IC 50 values of 2.54 and 4.53 μM. The structure‐activity relationships (SARs) study indicated that the introduction of dibenzyl ether, substituted silyl and long chain aliphatic‐triazoles at C‐10 position of genipin were most effective in improving cytotoxicity. Molecular docking results provided the information for further modification of genipin scaffold for development as cytotoxic agent.
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