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特级初榨橄榄油中的酚类次级胆汁酸抑制纤维生成和致癌上皮-间充质转化:特级初榨橄榄油作为新型抗衰老植物化学物质的来源。

Phenolic secoiridoids in extra virgin olive oil impede fibrogenic and oncogenic epithelial-to-mesenchymal transition: extra virgin olive oil as a source of novel antiaging phytochemicals.

机构信息

Catalan Institute of Oncology , Girona, Catalonia, Spain.

出版信息

Rejuvenation Res. 2012 Feb;15(1):3-21. doi: 10.1089/rej.2011.1203. Epub 2012 Jan 9.

DOI:10.1089/rej.2011.1203
PMID:22229524
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3283896/
Abstract

The epithelial-to-mesenchymal transition (EMT) genetic program is a molecular convergence point in the life-threatening progression of organ fibrosis and cancer toward organ failure and metastasis, respectively. Here, we employed the EMT process as a functional screen for testing crude natural extracts for accelerated drug development in fibrosis and cancer. Because extra virgin olive oil (EVOO) (i.e., the juice derived from the first cold pressing of the olives without any further refining process) naturally contains high levels of phenolic compounds associated with the health benefits derived from consuming an EVOO-rich Mediterranean diet, we have tested the ability of an EVOO-derived crude phenolic extract to regulate fibrogenic and oncogenic EMT in vitro. High-performance liquid chromatography (HPLC) coupled to time-of-flight (TOF) mass spectrometry assays revealed that the EVOO phenolic extract was mainly composed (∼70%) of two members of the secoiridoid family of complex polyphenols, namely oleuropein aglycone-the bitter principle of olives-and its derivative decarboxymethyl oleuropein aglycone. EVOO secoiridoids efficiently prevented loss of proteins associated with polarized epithelial phenotype (i.e., E-cadherin) as well as de novo synthesis of proteins associated with mesenchymal migratory morphology of transitioning cells (i.e., vimentin). The ability of EVOO to impede transforming growth factor-β (TGF-β)-induced disintegration of E-cadherin-mediated cell-cell contacts apparently occurred as a consequence of the ability of EVOO phenolics to prevent the upregulation of SMAD4-a critical mediator of TGF-β signaling-and of the SMAD transcriptional cofactor SNAIL2 (Slug)-a well-recognized epithelial repressor. Indeed, EVOO phenolics efficiently prevented crucial TGF-β-induced EMT transcriptional events, including upregulation of SNAI2, TCF4, VIM (Vimentin), FN (fibronectin), and SERPINE1 genes. While awaiting a better mechanistic understanding of how EVOO phenolics molecularly shut down the EMT differentiation process, it seems reasonable to suggest that nontoxic Oleaceae secoiridoids certainly merit to be considered for aging studies and, perhaps, for ulterior design of more pharmacologically active second-generation anti-EMT molecules.

摘要

上皮-间充质转化 (EMT) 遗传程序是器官纤维化和癌症分别向器官衰竭和转移的致命进展过程中的分子汇聚点。在这里,我们将 EMT 过程用作功能筛选,以测试粗天然提取物在纤维化和癌症中的加速药物开发。因为特级初榨橄榄油 (EVOO)(即未经任何进一步精炼过程从橄榄中第一次冷榨获得的汁液)天然含有高水平的酚类化合物,这些化合物与从富含特级初榨橄榄油的地中海饮食中获得的健康益处有关,因此我们测试了 EVOO 衍生的粗酚提取物调节体外纤维生成和致癌 EMT 的能力。高效液相色谱 (HPLC) 与飞行时间 (TOF) 质谱联用分析表明,EVOO 酚提取物主要由复杂多酚的 secoiridoid 家族的两个成员组成,即橄榄苦苷 - 橄榄的苦味成分 - 和它的衍生物去羧甲基橄榄苦苷。EVOO secoiridoids 有效地防止与极化上皮表型相关的蛋白质的丢失(即 E-钙粘蛋白)以及与过渡细胞的间质迁移形态相关的新合成蛋白质(即波形蛋白)。EVOO 阻止转化生长因子-β (TGF-β) 诱导的 E-钙粘蛋白介导的细胞-细胞接触解体的能力显然是由于 EVOO 酚类能够阻止 TGF-β 信号转导的关键介质 SMAD4 和 SMAD 转录共因子 SNAIL2(Slug)的上调而发生的- 一种公认的上皮抑制剂。事实上,EVOO 酚类有效地阻止了关键的 TGF-β 诱导的 EMT 转录事件,包括 SNAI2、TCF4、VIM(波形蛋白)、FN(纤连蛋白)和 SERPINE1 基因的上调。虽然我们还在等待更好地了解 EVOO 酚类如何从分子上关闭 EMT 分化过程,但似乎可以合理地建议无毒的木犀科 secoiridoids 肯定值得考虑用于衰老研究,也许还可以进一步设计更具药理活性的第二代抗 EMT 分子。

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