In the present work, a small library of few 1-deoxysphingolipid ceramides has been designed and synthesized via an efficient UGI multicomponent reaction. The deoxy sphingosine intermediate (10) synthesized via Grignard reaction and olefin metathesis reaction was used as the amine component with cyclohexyl isocyanide and various aldehydes. The butyric acid has been used as an acid component which may turn out be an advantage due to the chemo preventive properties of the acid formed after the partial hydrolysis of the ceramide. Compounds (1-6) has been synthesised via a short and facile route in high purity and yield. Molecular docking of all the analogues has been carried out with protein Sphingosine Kinase I using BiopredictaVlife MDS tool to determine the relative docking score and ligand-protein interactions. Further in vitro studies were performed on PC-3 (prostate cancer) and HCT-116 (colon cancer) cell lines in which four compounds (1-4) showed reasonable anti-cancer activity against both the cell lines while compound (3) showed highest activity with IC50 value of 0.344 mu M against PC-3 (prostate cancer) cell lines and 0.624 mu M against HCT-116 (colon cancer) cell lines. Compound (4) showed IC50 value of 0.472 mu M against HCT-116 (colon cancer) cell lines.
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机译:在本工作中,通过高效的UGI多组分反应设计并合成了少量1-脱氧鞘脂神经酰胺的小型库。以格氏反应和烯烃复分解反应合成的脱氧鞘氨醇中间体(10)作为胺组分,与环己基异氰酸化物和各种醛类化合物共成。丁酸已被用作酸成分,由于神经酰胺部分水解后形成的酸的化学预防特性,这可能是一个优势。化合物 (1-6) 已通过短而简单的路线合成,纯度高,收率高。使用 BiopredictaVlife MDS 工具与蛋白质鞘氨醇激酶 I 进行所有类似物的分子对接,以确定相对对接评分和配体-蛋白质相互作用。对PC-3(前列腺癌)和HCT-116(结肠癌)细胞系进行了进一步的体外研究,其中四种化合物(1-4)对两种细胞系都显示出合理的抗癌活性,而化合物(3)显示出最高的活性,对PC-3(前列腺癌)细胞系的IC50值为0.344μ M,对HCT-116(结肠癌)细胞系的IC50值为0.624μM。化合物(4)对HCT-116(结肠癌)细胞系的IC50值为0.472μM。
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