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首页> 外文期刊>Dalton transactions: An international journal of inorganic chemistry >Dual-acting antitumor Pt(IV) prodrugs of kiteplatin with dichloroacetate axial ligands
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Dual-acting antitumor Pt(IV) prodrugs of kiteplatin with dichloroacetate axial ligands

机译:双作用抗肿瘤PT(IV)与二氯乙酸二氯乙酯轴向配体的KITEPLATIN前药

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摘要

With the aim to obtain dual acting drugs able to target both nuclear DNA and mitochondria, Pt(iv) kiteplatin derivatives having dichloroacetate (DCA) ligands in axial positions have been synthesized. The rather fast hydrolysis (t(1/2) of ca. 1 h) and reduction (by ascorbic acid) of these Pt(iv) derivatives did not impede a potent pharmacological effect on tumor cells. Moreover, similarly to kiteplatin, also the Pt(iv)-DCA compounds proved to be capable of overcoming oxaliplatin-resistance, which is particularly important in view of the fact that metastatic colorectal cancer is the third most common cancer in males and the second in females. The possible role of DCA released by the Pt(iv) compounds in eliciting the antiproliferative activity has also been investigated. Pt(iv)-DCA compounds determine a substantial increase of ROS production, blockage of oxidative phosphorylation, hypopolarization of the mitochondrial membrane, and caspase-3/7 mediated apoptotic cell death.
机译:通过旨在获得能够靶向核DNA和线粒体的双作用药物,已经合成了具有二氯乙酸二氯酸酯(DCA)配体的PT(IV)KITEPLATIN衍生物已经合成。 这些PT(IV)衍生物的Ca.1H)和Ca.1h)和还原(抗坏血酸)的相当快的水解(抗坏血酸)并未阻碍肿瘤细胞的有效药理学作用。 此外,类似于KITEPLATIN,也证明了PT(IV)-DCA化合物能够克服奥沙利铂耐药性,这鉴于转移性结直肠癌是男性第三次常见的癌症和第二次常见癌症尤其重要 女性。 还研究了Pt(iv)化合物在引发抗增殖活性时释放的DCA的可能作用。 Pt(IV)-DCA化合物决定了ROS生产的大量增加,氧化磷酸化,线粒体膜的低聚化,以及Caspase-3/7介导的凋亡细胞死亡。

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