Shiau Jeng-Yuan, Chang Yong-Qun, Nakagawa-Goto Kyoko, Lee Kuo-Hsiung, Shyur Lie-Fen
Institute of Biotechnology, National Taiwan UniversityTaipei, Taiwan.
Agricultural Biotechnology Research Center, Academia SinicaTaipei, Taiwan.
Front Pharmacol. 2017 Jun 29;8:398. doi: 10.3389/fphar.2017.00398. eCollection 2017.
A novel plant sesquiterpene lactone derivative, DET derivative (DETD)-35, originating from parental deoxyelephantopin (DET) was previously observed to effectively suppress human triple negative breast cancer (TNBC) MDA-MB-231 cell activity and tumor growth in mice. In this study, the mechanisms underlying the activity of DETD-35 were elucidated. DET and DETD-35 induced reactive oxygen species (ROS) which caused structural damage and dysfunction of mitochondria and increased cytosolic calcium level, subsequently evoking exosome release from the cancer cells. Intriguingly, exosomes induced by both compounds had an atypical function. Cancer cell-derived exosomes commonly show metastatic potential, but upon DET/DETD-35 treatment exosomes showed anti-proliferative activity against MDA-MB-231 cells. Quantitative proteome analysis of TNBC cell-secreted exosomes showed that DET and DETD-35 attenuated the expression of proteins related to cell migration, cell adhesion, and angiogenesis. Furthermore, several exosomal proteins participating in biological mechanisms such as oxidative stress and decrease of transmembrane potential of mitochondria were found deregulated by treatment with either compound. Pretreatment with ROS scavenger, -acetylcysteine, blockaded DET- or DETD-35-induced oxidative stress and calcium dependent exosome release mechanisms, and also reverted DET- or DETD-35-induced reprogramming exosomal protein expression profiles resulting in attenuation of exosomal toxicity against TNBC cell proliferation. In summary, this study shows that a plant-derived sesquiterpene lactone DET and its analog DETD-35 inhibitory TNBC cell activities through oxidative stress-induced cancer cell releasing exosomes in tandem with alteration of exosomal protein composition and functions. The findings of this study suggest that DETD-35 may be suitable for further development into an anti-TNBC drug.
一种源自亲本脱氧地胆草素(DET)的新型植物倍半萜内酯衍生物,即DET衍生物(DETD)-35,先前已观察到其能有效抑制人三阴性乳腺癌(TNBC)MDA-MB-231细胞活性及小鼠肿瘤生长。在本研究中,阐明了DETD-35活性的潜在机制。DET和DETD-35诱导活性氧(ROS)生成,导致线粒体结构损伤和功能障碍,并提高胞质钙水平,随后引发癌细胞释放外泌体。有趣的是,这两种化合物诱导的外泌体具有非典型功能。癌细胞衍生的外泌体通常具有转移潜能,但经DET/DETD-35处理后,外泌体对MDA-MB-231细胞表现出抗增殖活性。对TNBC细胞分泌的外泌体进行定量蛋白质组分析表明,DET和DETD-35减弱了与细胞迁移、细胞黏附和血管生成相关的蛋白质表达。此外,发现几种参与氧化应激和线粒体跨膜电位降低等生物学机制的外泌体蛋白因任一化合物处理而失调。用ROS清除剂N-乙酰半胱氨酸预处理可阻断DET或DETD-35诱导的氧化应激和钙依赖性外泌体释放机制,还可逆转DET或DETD-35诱导的外泌体蛋白质表达谱重编程,从而减弱外泌体对TNBC细胞增殖的毒性。总之,本研究表明,一种植物源倍半萜内酯DET及其类似物DETD-35通过氧化应激诱导癌细胞释放外泌体,并同时改变外泌体蛋白质组成和功能来抑制TNBC细胞活性。本研究结果表明,DETD-35可能适合进一步开发为抗TNBC药物。
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