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首页> 外文期刊>Journal of biological inorganic chemistry: JBIC: a publication of the Society of Biological Inorganic Chemistry >Synthesis, Ti(IV) intake by apotransferrin and cytotoxic properties of functionalized titanocene dichlorides
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Synthesis, Ti(IV) intake by apotransferrin and cytotoxic properties of functionalized titanocene dichlorides

机译:载脂铁蛋白的合成,Ti(IV)的摄入及功能化二茂钛二氯化物的细胞毒性

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摘要

Functionalization of cyclopentadienyl (Cp) ligands and incorporation of these into a Ti(IV) center require careful design and selection of the appropriate synthetic routes to obtain the desired product in reasonably good yields. As part of our research efforts in the area of titanocene antitumor agents, we have revisited the synthesis of Cp rings with electron-withdrawing groups and their corresponding titanocene dichlorides, (Cp-R)(2)TiCl2 and (Cp-R)CpTiCl2, where R is CO2CH3 and CO2CH2CH3. These complexes were characterized by elemental analysis and H-1 and C-13 NMR and IR spectroscopies. This report presents the first detailed synthetic route for (Cp-CO2CH2CH3)CpTiCl2 and provides an alternate route for synthesis of (Cp-R)(2)TiCl2 complexes. The ability of these complexes to deliver Ti(IV) to apotransferrin was investigated to elucidate how the functionalized Cp ligands affect the titanium intake by apotransferrin. The subject complexes transfer Ti(IV) to human apotransferrin, loading both N- and C-lobes. The antitumor activity of these complexes against HT-29 cancer colon cells was determined using a 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide assay. Carboethoxy Cp functionalization results in complexes with a toxicity comparable to that of titanocene dichloride. The carbomethoxy-functionalized complexes proved to be nonactive at the time intervals studied here, regardless of their ability to donate the titanium atom to human apotransferrin.
机译:环戊二烯基(Cp)配体的功能化以及将它们并入Ti(IV)中心需要仔细设计和选择适当的合成途径,以合理的高收率获得所需的产品。作为我们在钛茂抗肿瘤剂领域研究工作的一部分,我们重新考虑了具有吸电子基团及其相应的钛茂二氯化物(Cp-R)(2)TiCl2和(Cp-R)CpTiCl2,其中R是CO 2 CH 3和CO 2 CH 2 CH 3。这些配合物通过元素分析,H-1和C-13 NMR和IR光谱进行表征。该报告介绍了(Cp-CO2CH2CH3)CpTiCl2的第一个详细的合成路线,并提供了(Cp-R)(2)TiCl2配合物的替代合成路线。研究了这些络合物将Ti(IV)传递至载铁蛋白的能力,以阐明功能化Cp配体如何影响载脂蛋白对钛的摄入。主体复合物将Ti(IV)转移至人载脂蛋白,同时加载N和C瓣。使用3-(4,5-二甲基噻唑-2-基)-2,5-二苯基四唑溴化物测定法测定这些复合物对HT-29癌细胞的抗肿瘤活性。碳乙氧基Cp官能化生成的复合物的毒性与二茂钛二氯化物的毒性相当。碳甲氧基官能化的络合物在本文研究的时间间隔证明是无活性的,无论其将钛原子捐赠给载脂蛋白的能力如何。

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