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Silylation Improves the Photodynamic Activity of Tetraphenylporphyrin Derivatives In Vitro and In Vivo

机译:甲硅烷基化可提高四苯基卟啉衍生物的体内和体外光动力学活性

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摘要

The effects of silyl and hydrophilic groups on the photodynamic properties of tetraphenylporphyrin (TPP) derivatives have been studied in vitro and in vivo. Silylation led to an improvement in the quantum yield of singlet oxygen sensitization for both sulfo and carboxy derivatives, although the silylation did not affect other photophysical properties. Silylation also improved the cellular uptake efficiency for both sulfo and carboxy derivatives, enhancing the in vitro photodynamic activity of the photosensitizer in U251 human glioma cells. The carboxy derivative (SiTPPC_4) was found to show higher cellular uptake efficiency and in vitro photodynamic activity than the corresponding sulfo derivative (SiTPPS_4), which indicates that the carboxy group is a more promising hydrophilic group than the sulfo group in the silylated porphyrin. SiTPPC_4 was found to show high selective accumulation efficiency in tumors, although almost no tumor selectivity was observed for the nonsilylated porphyrin. The concentration of SiTPPC_4 in tumors was 13 times higher than that in muscle 12 h after drug administration. We also studied tumor response after treatment and found that silylation enhanced in vivo photodynamic activity significantly. SiTPPC_4 shows higher photodynamic activity than NPe6 with white light irradiation.
机译:甲硅烷基和亲水基团对四苯基卟啉(TPP)衍生物的光动力学性质的影响已在体外和体内进行了研究。甲硅烷基化导致磺基和羧基衍生物的单线态氧敏化的量子产率提高,尽管甲硅烷基化并不影响其他光物理性质。甲硅烷基化还提高了磺基和羧基衍生物的细胞吸收效率,增强了光敏剂在U251人神经胶质瘤细胞中的体外光动力活性。发现羧基衍生物(SiTPPC_4)比相应的磺基衍生物(SiTPPS_4)具有更高的细胞吸收效率和体外光动力活性,这表明羧基比甲硅烷基化的卟啉中的磺基更具有前景。尽管几乎未观察到未甲硅烷基化的卟啉对肿瘤的选择性,但发现SiTPPC_4在肿瘤中显示出高选择性积聚效率。给药后12小时,肿瘤中SiTPPC_4的浓度比肌肉中的浓度高13倍。我们还研究了治疗后的肿瘤反应,发现甲硅烷基化显着增强了体内的光动力活性。 SiTPPC_4在白光照射下显示出比NPe6高的光动力活性。

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