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Synthesis characterization and in-vitro antitumor activity of the polyethylene glycol (350 and 1000) succinate derivatives of the tocopherol and tocotrienol isomers of Vitamin E

机译:维生素E的生育酚和生育三烯酚异构体的聚乙二醇(350和1000)琥珀酸酯衍生物的合成表征和体外抗肿瘤活性

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摘要

Vitamin E refers to a group of saturated tocopherol (T) isomers and the biologically more active unsaturated tocotrienol (T3) isomers. PEGylated α-tocopherol, commercially known as Vitamin E TPGS, has been used as an emulsifier and therapeutic agent for children with vitamin E deficiency. Limited information, however, is available about the PEG conjugates of the tocotrienol isomers of vitamin E. The current work was therefore undertaken to synthesize and characterize the water soluble polyethylene glycol (PEG 350 and 1000) derivatives of T and T3. Yield and the identity of the synthesized products were confirmed by 1H NMR, mass spectroscopy, HPLC, and thermal analysis. The self-assembly of the PEGylated vitamin E isomers in water at critical micelle concentrations (CMC) was further confirmed by size, zeta, and Cryo-TEM image analysis. While stable at pH 7.4, PEG conjugates were found to rapidly hydrolyze at pH 1.2. Our data showed that PEGylated T3 isomers were significantly more active as inhibitors for P-glycoprotein than PEGylated T. The in vitro cytotoxicity of the conjugates was also tested against a large panel of normal and tumorigenic cells. Of the conjugates, γ-T3PGS 1000 and δ-T3PGS 1000 were found to have the least toxicity against non-tumorigenic breast and pancreatic cell lines, which may be advantageous for its use as functional excipients in drug delivery. The results from the current work have demonstrated the feasibility of synthesizing PEGylated conjugates of vitamin E isomers and highlighted the potential use of these conjugates in drug delivery as functional and safer excipients especially for γ-T3PGS 1000 and δ-T3PGS 1000 conjugate.
机译:维生素E是指一组饱和的生育酚(T)异构体和生物学上更具活性的不饱和生育三烯酚(T3)异构体。聚乙二醇化的α-生育酚,商业上称为维生素E TPGS,已经被用作维生素E缺乏症儿童的乳化剂和治疗剂。但是,关于维生素E的生育三烯酚异构体的PEG共轭物的信息有限。因此,目前正在进行的工作是合成和表征T和T3的水溶性聚乙二醇(PEG 350和1000)衍生物。通过 1 1 H NMR,质谱,HPLC和热分析确认了合成产物的产率和身份。通过大小,ζ和Cryo-TEM图像分析,进一步证实了临界胶束浓度(CMC)下水中PEG化维生素E异构体的自组装。虽然在pH 7.4下稳定,但发现PEG共轭物在pH 1.2下迅速水解。我们的数据表明,聚乙二醇化的T3异构体作为P-糖蛋白抑制剂的活性明显高于聚乙二醇化的T。对缀合物的体外细胞毒性也针对大量正常细胞和致瘤细胞进行了测试。在缀合物中,发现γ-T3PGS1000和δ-T3PGS1000对非致瘤性乳腺和胰腺细胞系的毒性最小,这可能有利于在药物递送中用作功能性赋形剂。当前工作的结果证明了合成维生素E异构体的PEG化缀合物的可行性,并强调了这些缀合物作为功能性和安全性赋形剂在药物递送中的潜在用途,尤其是对于γ-T3PGS1000和δ-T3PGS1000缀合物。

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