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Nanoscale Reaction Vessels Designed for Synthesis of Copper-Drug Complexes Suitable for Preclinical Development

机译:设计用于合成适合临床前开发的铜-药物配合物的纳米级反应容器

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摘要

The development of copper-drug complexes (CDCs) is hindered due to their very poor aqueous solubility. Diethyldithiocarbamate (DDC) is the primary metabolite of disulfiram, an approved drug for alcoholism that is being repurposed for cancer. The anticancer activity of DDC is dependent on complexation with copper to form copper bis-diethyldithiocarbamate (Cu(DDC)(2)), a highly insoluble complex that has not been possible to develop for indications requiring parenteral administration. We have resolved this issue by synthesizing Cu(DDC)(2) inside liposomes. DDC crosses the liposomal lipid bilayer, reacting with the entrapped copper; a reaction that can be observed through a colour change as the solution goes from a light blue to dark brown. This method is successfully applied to other CDCs including the anti-parasitic drug clioquinol, the natural product quercetin and the novel targeted agent CX-5461. Our method provides a simple, transformative solution enabling, for the first time, the development of CDCs as viable candidate anticancer drugs; drugs that would represent a brand new class of therapeutics for cancer patients.
机译:铜-药物复合物(CDC)的开发由于其水溶性很差而受到阻碍。二乙基二硫代氨基甲酸酯(DDC)是双硫仑的主要代谢产物,双硫仑是一种批准用于酒精中毒的药物,现已重新用于癌症。 DDC的抗癌活性取决于与铜的络合形成双二乙基二硫代氨基甲酸铜(Cu(DDC)(2)),这是一种高度不溶的复合物,无法用于需要肠胃外给药的适应症。我们已经通过合成脂质体内的Cu(DDC)(2)解决了这个问题。 DDC穿过脂质体脂质双层,与包裹的铜反应;当溶液从浅蓝色变为深棕色时,可以通过颜色变化观察到这种反应。该方法已成功应用于其他CDC,包括抗寄生虫药物氯喹醇,天然产物槲皮素和新型靶向药物CX-5461。我们的方法提供了一种简单的转化解决方案,首次使CDC成为可行的候选抗癌药物。代表癌症患者全新治疗方法的药物。

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