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首页> 外文期刊>Cancer Cell International >Cycloartane-3,24,25-triol inhibits MRCKα kinase and demonstrates promising anti prostate cancer activity in vitro
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Cycloartane-3,24,25-triol inhibits MRCKα kinase and demonstrates promising anti prostate cancer activity in vitro

机译:Cycloartane-3,24,25-triol抑制MRCKα激酶并在体外表现出有希望的抗前列腺癌活性

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Background Given the high occurrence of prostate cancer worldwide and one of the major sources of the discovery of new lead molecules being medicinal plants, this research undertook to investigate the possible anti-cancer activity of two natural cycloartanes; cycloartane-3,24,25-diol (extracted in our lab from Tillandsia recurvata) and cycloartane-3,24,25-triol (purchased). The inhibition of MRCKα kinase has emerged as a potential solution to restoring the tight regulation of normal cellular growth, the loss of which leads to cancer cell formation. Methods Kinase inhibition was investigated using competition binding (to the ATP sites) assays which have been previously established and authenticated and cell proliferation was measured using the WST-1 assay. Results Cycloartane-3,24,25-triol demonstrated strong selectivity towards the MRCKα kinase with a Kd50 of 0.26 μM from a total of 451 kinases investigated. Cycloartane-3,24,25-triol reduced the viability of PC-3 and DU145 cell lines with IC50 values of 2.226?±?0.28 μM and 1.67?±?0.18 μM respectively. Conclusions These results will prove useful in drug discovery as Cycloartane-3,24,25-triol has shown potential for development as an anti-cancer agent against prostate cancer.
机译:背景技术鉴于世界范围内前列腺癌的高发以及新的先导分子是药用植物的发现的主要来源之一,本研究致力于研究两种天然环烷的可能的抗癌活性。环烷3,24,25-二醇(在我们的实验室中从铁兰提取)和环烷3,24,25-三醇(购买)。抑制MRCKα激酶已成为恢复正常细胞生长的严格调节的潜在解决方案,这种丧失会导致癌细胞的形成。方法使用竞争结合(与ATP位点结合)测定法研究激酶抑制作用,该测定法先前已建立并通过鉴定,并且使用WST-1测定法测定细胞增殖。结果Cycloartane-3,24,25-triol对MRCKα激酶具有很强的选择性,Kd 50 为0.26μM,来自总共451种激酶。 Cycloartane-3,24,25-triol降低了PC-3和DU145细胞系的生存能力,IC 50 值分别为2.226±0.28μM和1.67±0.18μM。结论这些结果将证明在药物开发中有用,因为Cycloartane-3,24,25-triol已显示出作为抗前列腺癌抗癌药的潜力。

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