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Oxidative Stress, DNA, Cell Cycle/Cell Cycle Associated Proteins and Multidrug Resistance Proteins: Targets of Human Amniotic Membrane in Hepatocellular Carcinoma

机译:氧化应激,DNA,细胞周期/细胞周期相关蛋白和多药耐药蛋白:肝细胞癌中人羊膜的目标。

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摘要

The anticancer effects of human amniotic membrane (hAM) have been studied over the last decade. However, the action mechanisms responsible for these effects are not fully understood until now. Previously results reported by our team proved that hAM is able to induce cytotoxicity and cell death in hepatocellular carcinoma (HCC), a worldwide high incident and mortal cancer. Therefore, this experimental study aimed to investigate the cellular targets of hAM protein extracts (hAMPE) in HCC through in vitro studies. Our results showed that hAMPE is able to modify oxidative stress environment in all HCC cell lines, as well as its cell cycle. hAMPE differently targets deoxyribonucleic acid (DNA), P21, P53, beta-catenin and multidrug resistance (MDR) proteins in HCC cell lines. In conclusion, hAMPE has several targets in HCC, being clear that the success of this treatment depends of a personalized therapy based on the biological and genetic characteristics of the tumor.
机译:在过去的十年中,已经研究了人类羊膜(hAM)的抗癌作用。但是,到目前为止,尚未完全了解引起这些作用的作用机制。我们小组先前报告的结果证明,hAM能够诱导肝细胞癌(HCC)(一种全球性高发和致命癌症)的细胞毒性和细胞死亡。因此,本实验研究旨在通过体外研究来研究肝癌中hAM蛋白提取物(hAMPE)的细胞靶标。我们的结果表明,hAMPE能够改变所有HCC细胞系的氧化应激环境及其细胞周期。 hAMPE以不同的方式靶向HCC细胞系中的脱氧核糖核酸(DNA),P21,P53,β-连环蛋白和多药耐药性(MDR)蛋白。总之,hAMPE在HCC中具有多个靶标,很明显,这种治疗方法的成功取决于基于肿瘤生物学和遗传特征的个性化治疗。

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