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Anticancer Applications of Nanostructured Silica-Based Materials Functionalized with Titanocene Derivatives: Induction of Cell Death Mechanism through TNFR1 Modulation

机译:钛新世衍生物功能化的纳米结构二氧化硅基材料的抗癌应用:通过TNFR1调节诱导细胞死亡机制。

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摘要

A series of cytotoxic titanocene derivatives have been immobilized onto nanostructured silica-based materials using two different synthetic routes, namely, (i) a simple grafting protocol via protonolysis of the Ti–Cl bond; and (ii) a tethering method by elimination of ethanol using triethoxysilyl moieties of thiolato ligands attached to titanium. The resulting nanostructured systems have been characterized by different techniques such as XRD, XRF, DR-UV, BET, SEM, and TEM, observing the incorporation of the titanocene derivatives onto the nanostructured silica and slight changes in the textural features of the materials after functionalization with the metallodrugs. A complete biological study has been carried out using the synthesized materials exhibiting moderate cytotoxicity in vitro against three human hepatic carcinoma (HepG2, SK-Hep-1, Hep3B) and three human colon carcinomas (DLD-1, HT-29, COLO320) and very low cytotoxicity against normal cell lines. In addition, the cells’ metabolic activity was modified by a 24-h exposure in a dose-dependent manner. Despite not having a significant effect on TNFα or the proinflammatory interleukin 1α secretion, the materials strongly modulated tumor necrosis factor (TNF) signaling, even at sub-cytotoxic concentrations. This is achieved mainly by upregulation of the TNFR1 receptor production, something which has not previously been observed for these systems.
机译:已经使用两种不同的合成途径将一系列细胞毒性钛茂衍生物固定在纳米结构的二氧化硅基材料上,即:(i)通过Ti-Cl键的质子分解进行简单的接枝​​; (ii)通过使用连接至钛的硫醇基配体的三乙氧基甲硅烷基部分消除乙醇来进行束缚的方法。所得的纳米结构体系已通过不同技术(例如XRD,XRF,DR-UV,BET,SEM和TEM)进行了表征,观察到钛茂衍生物已掺入纳米结构二氧化硅中并在功能化后材料的结构特征发生了细微变化与金属药物。使用合成的材料对三种人类肝癌(HepG2,SK-Hep-1,Hep3B)和三种人类结肠癌(DLD-1,HT-29,COLO320)具有体外中度细胞毒性的合成材料已进行了完整的生物学研究。对正常细胞系的细胞毒性非常低。另外,细胞的代谢活性通过剂量依赖性的24小时暴露而改变。尽管这些物质对TNFα或促炎性白介素1α的分泌没有显着影响,但即使在亚细胞毒性浓度下,该材料仍能强烈调节肿瘤坏死因子(TNF)信号传导。这主要是通过上调TNFR1受体的产量来实现的,而这在这些系统中以前还没有观察到。

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