钌衍生化合物的合成、表征及其在MCF-7细胞中抗肿瘤潜力的评估

Moraes Fabricio Tarso, Galvão Anderson Dourado, F. D. Batista, Amorin Kelly Aparecida da Encarnação, Sousa Claudia Cristina, H. Cristina, França Eduardo Luzia, Costa Daniel Tizo, S. Batista
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引用次数: 0

摘要

为了合成、表征和评估钌化合物的抗肿瘤潜力,本研究从前体K[RuCl4(bipy)]中产生了一种简单且可重复的合成Ru+3与bipy和L-trip配位的新化合物的途径。中红外区(FTIR)的光谱表征显示了Ru-(L-trip)之间的相互作用,通过羧酸根离子带对更高能量的位移以及脂肪胺带的位移证明了这一点,表明L-trip配体发生了双齿配位。用热分析技术获得的结果的分析表明,化合物的最小化学式[RuCl2(bipy)(L-trip)]1/2H2O。对前体K[RuCl4(bipy)]的抗肿瘤潜力的评估显示出对MCF-7细胞系的毒性作用,但没有显示出选择性,并且没有达到相同程度的PBMC细胞。对新合成的化合物[RuCl2(bipy)(L-trip)]的抗肿瘤潜力的评估表明,与PBMC细胞相比,将L-色氨酸分子插入前体配位球使其对MCF-7型肿瘤细胞具有选择性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Synthesis, Characterization, and Evaluation of Antitumor Potential in MCF-7 Cells of Ruthenium-Derived Compounds
To synthesize, characterize and evaluate the antitumor potential derived from ruthenium compounds was generated in this study, from the precursor K[RuCl4(bipy)] a route in a simple and reproducible synthesis for a novel compound of coordinating Ru+3 with bipy and L-trip. The spectroscopic characterization in the middle infrared region (FTIR) shows the interactions between Ru-(L-trip), evidenced by the displacement of the carboxylate ion band for higher energies, and also by the displacements of aliphatic amine bands, suggesting that bidentate coordination of the L-trip ligand occurred. Analysis of the results obtained with thermoanalytical techniques showed that the minimum formula of the compound, [RuCl2(bipy)(L-trip)]1/2H2O. Evaluation of the antitumor potential of precursor K[RuCl4(bipy)] showed the toxic effects on MCF-7 cell line, but did not show selectivity and not reached PBMC cells to the same extent. The evaluation of the antitumor potential of the newly synthesized compound, [RuCl2(bipy)(L-trip)], demonstrated that the insertion of an L-tryptophan molecule into the precursor coordination sphere made it selective when compared to PBMC cells, for MCF-7 type tumor cells.
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