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首页> 外文期刊>ChemMedChem >Novel 4-Amino Bis-pyridinium and Bis-quinolinium Derivatives as Choline Kinase Inhibitors with Antiproliferative Activity against the Human Breast Cancer SKBR-3 Cell Line
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Novel 4-Amino Bis-pyridinium and Bis-quinolinium Derivatives as Choline Kinase Inhibitors with Antiproliferative Activity against the Human Breast Cancer SKBR-3 Cell Line

机译:新型的4-氨基双吡啶和双喹啉鎓衍生物作为胆碱激酶抑制剂对人乳腺癌SKBR-3细胞系具有抗增殖活性

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摘要

Choline kinase (ChoK) is the first enzyme in the CDP-choline pathway that synthesizes phosphatidylcholine, the major phospholipid in eukaryotic cell membranes. Human ChoK has three isoforms: ChoKα1, α2, and β Specific inhibition of ChoKα has been reported to selectively kill tumor cells. In this study, ten new symmetrical bis-pyridinium and bis-quinolinium derivatives were synthesized and tested for their ability to inhibit human ChoKα2. These compounds have electron-releasing groups at position 4 of the pyridinium or quinolinium rings. 1,1'-f(Butane-1,3-diylbis(benzene-1,4-diylmethylene)]bis[4-(4-bromo-N-methylanilino)pyridinium)] dibromide and 1,1'-(bi-phenyl-3,3'-diylmethylene)bis[7-chloro-4-(perhydroazepine-1-yl)quinolinium] dibromide were identified as highly potent ChoK inhibitors with IC_(50) values of 80 nM. Kinetic enzymatic assays indicated a mixed and predominantly competitive mechanism of inhibition for these compounds, which exhibited strong antiproliferative activity (EC_(50) 1 μm) against the human breast cancer SKBR3 cell line.
机译:胆碱激酶(ChoK)是CDP-胆碱途径中的第一种酶,可合成磷脂酰胆碱,这是真核细胞膜中的主要磷脂。人ChoK具有三种亚型:ChoKα1,α2和β。据报道,对ChoKα的特异性抑制作用可选择性杀死肿瘤细胞。在这项研究中,合成了十种新的对称双吡啶和双喹啉鎓衍生物,并测试了它们抑制人ChoKα2的能力。这些化合物在吡啶鎓或喹啉鎓环的4位具有电子释放基团。 1,1'-f(丁烷1,3,2-二基双(苯-1,4-二基亚甲基)]双[4-(4-溴-N-甲基苯胺基)吡啶鎓]]二溴化物和1,1'-(二-苯基-3,3'-二基亚甲基)双[7-氯-4-(全氢氮杂-1-基)喹啉鎓]二溴化物被确定为高效的ChoK抑制剂,IC_(50)值为80 nM。动力学酶分析表明对这些化合物的抑制作用的混合和主要竞争机制,对人乳腺癌SKBR3细胞系表现出强大的抗增殖活性(EC_(50)1μm)。

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