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γ-和δ-生育三烯酚干扰衰老,导致细胞活力下降。

γ- and δ-Tocotrienols interfere with senescence leading to decreased viability of cells.

机构信息

Faculty of Medicine, Institute of Medical Chemistry, Biochemistry and Clinical Biochemistry, Comenius University, Bratislava, Slovakia.

Jessenius Faculty of Medicine, Department of Medical Biochemistry, Comenius University, Bratislava, Martin, Slovakia.

出版信息

Mol Cell Biochem. 2021 Feb;476(2):897-908. doi: 10.1007/s11010-020-03954-w. Epub 2020 Oct 30.

Abstract

Senescence is an irreversible permanent cell cycle arrest accompanied by changes in cell morphology and physiology. Bioactive compounds including tocotrienols (vitamin E) can affect important biological functions. The aim of this study was to investigate how γ- and δ-tocotrienols can affect stress-induced premature senescence. We established two different models of premature stress senescence by induction of senescence with either hydrogen peroxide or etoposide in human lung fibroblasts MRC-5 (ECACC, England). We observed increased percentage of cells with increased SA-β-galactosidase activity, decreased cell viability/proliferation and increased level of p21 in both models. In addition, γ-tocotrienol or δ-tocotrienol (both at concentrations of 150, 200 and 300 μM) were added to the cells along with the inductor of senescence (cotreatment). We have found that this cotreatment led to the decrease of cell viability/proliferation in both models of premature stress senescence, but did not change the percentage of senescent cells. Moreover, we detected no expression of caspase-3 or apoptotic DNA fragmentation in any models of premature stress senescence after the cotreatment with γ- as well as δ-tocotrienols. However, an increased level of autophagic protein LC-3 II was detected in cells with hydrogen peroxide-induced senescence after the cotreatment with γ-tocotrienol as well as δ-tocotrienol. In case of etoposide-induced senescence only δ-tocotrienol cotreatment led to an increased level of LC-3 II protein in cells. According to our work δ-tocotrienol is more effective compound than γ-tocotrienol.

摘要

衰老(Senescence)是一种不可逆的永久性细胞周期停滞,伴随着细胞形态和生理的变化。生物活性化合物,包括生育三烯酚(维生素 E),可以影响重要的生物学功能。本研究的目的是研究γ-和δ-生育三烯酚如何影响应激诱导的早衰。我们通过过氧化氢或依托泊苷诱导人肺成纤维细胞 MRC-5(ECACC,英国)衰老,建立了两种不同的早衰应激模型。我们观察到两种模型中,SA-β-半乳糖苷酶活性增加的细胞比例增加,细胞活力/增殖减少,p21 水平升高。此外,γ-生育三烯酚或 δ-生育三烯酚(浓度均为 150、200 和 300 μM)与衰老诱导剂(共处理)一起添加到细胞中。我们发现,这种共处理导致两种早衰应激模型中细胞活力/增殖减少,但不改变衰老细胞的比例。此外,在用 γ-和 δ-生育三烯酚共处理后,在任何一种早衰应激模型中均未检测到 caspase-3 的表达或凋亡 DNA 片段的断裂。然而,在用过氧化氢诱导衰老的细胞中,在用 γ-生育三烯酚和 δ-生育三烯酚共处理后,检测到自噬蛋白 LC-3 II 的水平增加。在依托泊苷诱导的衰老中,只有 δ-生育三烯酚共处理导致细胞中 LC-3 II 蛋白水平增加。根据我们的研究,δ-生育三烯酚比 γ-生育三烯酚更有效。

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