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首页> 外文期刊>Journal of Heterocyclic Chemistry: The International Journal of Heterocyclic Chemistry >Synthesis of Novel Alkyl Amide Functionalized Trifluoromethyl Substituted Furo/thieno Pyridine Derivatives: Their Anticancer Activity and CoMFA and CoMSIA Studies
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Synthesis of Novel Alkyl Amide Functionalized Trifluoromethyl Substituted Furo/thieno Pyridine Derivatives: Their Anticancer Activity and CoMFA and CoMSIA Studies

机译:新型烷基酰胺的合成官能化三氟甲基取代呋喃/噻吩吡啶衍生物:抗癌活性和COMFA和COMSIA研究

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摘要

A series of novel alkyl amide functionalized trifluoromethyl substituted furo/thieno pyridine derivatives 4a-h, 5a-d, and 6a-h were prepared starting from 2-oxo/thioxo-6-phenyl/thien-2-yl-4-(trifluoromethyl)-1,2-dihydropyridine-3-carbonitrile 1 on reaction with bromoethylacetate followed by reaction with different primary aliphatic amines, cyclic secondary amines, or l-amino acids under different set of conditions. All the synthesized compounds 4a-h, 5a-d, and 6a-h were screened for anticancer activity against four cancer cell lines such as HeLa-cervical cancer (CCL-2), COLO205-colon cancer (CCL-222), HepG2-liver cancer (HB-8065), and MCF7-breast cancer (HTB-22). Compounds 4g and 4h are found to have promising anticancer activity at micromolar concentration. CoMFA and CoMSIA methods were applied to derive 3D-QSAR models for alkyl amide tagged furo/thieno pyridine derivatives as potential anticancer inhibitors. 3D-QSAR models provided a strong basis for future rational design of more active and selective HeLa, COLO205, HepG2, and MCF-7 cell line inhibitors.
机译:一系列新的烷基酰胺官能化三氟甲基取代的呋喃/噻吩吡啶衍生物4a-h,5a-d和6a-h是从2-氧代/硫代-6-苯基/噻吩-2-基4-(三氟甲基)-1,2-二氢吡啶-3-碳腈1与溴乙酸反应,然后与不同的初级脂族胺,环状仲胺或L-氨基酸在不同的条件下反应。筛选所有合成的化合物4a-h,5a-d和6a-h,用于针对四种癌细胞系(如hela-ccl-2),clo205-结肠癌(ccl-222),hepg2-肝癌(HB-8065)和MCF7-乳腺癌(HTB-22)。发现化合物4G和4H在微摩尔浓度下具有有前途的抗癌活性。应用COMFA和COMSIA方法对烷基酰胺的3D QSAR模型标记为呋喃/噻吩吡啶衍生物作为潜在的抗癌抑制剂。 3D-QSAR模型为未来的更具活跃和选择性HELA,COLO205,HEPG2和MCF-7细胞系抑制剂提供了强有力的基础。

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