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Synergistic Anticancer Effect of Tocotrienol Combined with Chemotherapeutic Agents or Dietary Components: A Review

机译:生育三烯酚与化学治疗剂或饮食成分联合的协同抗癌作用:综述

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Tocotrienol (T3), unsaturated vitamin E, is gaining a lot of attention owing to its potent anticancer effect, since its efficacy is much greater than that of tocopherol (Toc). Various factors are known to be involved in such antitumor action, including cell cycle arrest, apoptosis induction, antiangiogenesis, anti-metastasis, nuclear factor-κB suppression, and telomerase inhibition. Owing to a difference in the affinity of T3 and Toc for the α-tocopherol transfer protein, the bioavailability of orally ingested T3 is lower than that of Toc. Furthermore, cellular uptake of T3 is interrupted by coadministration of α-Toc in vitro and in vivo. Based on this, several studies are in progress to screen for molecules that can synergize with T3 in order to augment its potency. Combinations of T3 with chemotherapeutic drugs (e.g., statins, celecoxib, and gefitinib) or dietary components (e.g., polyphenols, sesamin, and ferulic acid) exhibit synergistic actions on cancer cell growth and signaling pathways. In this review, we summarize the current status of synergistic effects of T3 and an array of agents on cancer cells, and discuss their molecular mechanisms of action. These combination strategies would encourage further investigation and application in cancer prevention and therapy.
机译:生育三烯酚(T3),不饱和维生素E,由于其有效的抗癌作用而倍受关注,因为它的功效远大于生育酚(Toc)的功效。已知多种因素参与这种抗肿瘤作用,包括细胞周期停滞,细胞凋亡诱导,抗血管生成,抗转移,核因子-κB抑制和端粒酶抑制。由于T3和Toc对α-生育酚转移蛋白的亲和力不同,所以口服摄取的T3的生物利用度低于Toc。此外,在体外和体内共同施用α-Toc可中断T3的细胞摄取。基于此,正在进行一些研究以筛选可以与T3协同作用以增强其效力的分子。 T3与化学治疗药物(例如他汀类药物,塞来昔布和吉非替尼)或饮食成分(例如多酚,芝麻素和阿魏酸)的组合对癌细胞的生长和信号通路具有协同作用。在这篇综述中,我们总结了T3和一系列药物对癌细胞的协同作用的当前状态,并讨论了其作用的分子机制。这些组合策略将鼓励进一步的研究和在癌症预防和治疗中的应用。

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