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Disulfiram-induced cytotoxicity and endo-lysosomal sequestration of zinc in breast cancer cells

机译:双硫仑诱导的乳腺癌细胞毒性和锌的溶酶体内螯合

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Disulfiram, a clinically used alcohol-deterrent has gained prominence as a potential anti-cancer agent due to its impact on copper-dependent processes. Few studies have investigated zinc effects on disulfiram action, despite it having high affinity for this metal. Here we studied the cytotoxic effects of disulfiram in breast cancer cells, and its relationship with both intra and extracellular zinc. MCF-7 and BT474 cancer cell lines gave a striking time-dependent biphasic cytotoxic response between 0.01 and 10 mu M disulfiram. Co-incubation of disulfiram with low-level zinc removed this effect, suggesting that availability of extracellular zinc significantly influences disulfiram efficacy. Live-cell confocal microscopy using fluorescent endocytic probes and the zinc dye Fluozin-3 revealed that disulfiram selectively and rapidly increased zinc levels in endo-lysosomes. Disulfiram also caused spatial disorganization of late endosomes and lysosomes, suggesting they are novel targets for this drug. This relationship between disulfiram toxicity and ionophore activity was consolidated via synthesis of a new disulfiram analog and overall we demonstrate a novel mechanism of disulfiram-cytotoxicity with significant clinical implications for future use as a cancer therapeutic. (C) 2015 The Authors. Published by Elsevier Inc.
机译:由于其对铜依赖性过程的影响,作为一种潜在的抗癌剂,临床上用于酒精抑制的双硫仑已经获得了广泛的关注。很少有研究调查锌对二硫仑作用的影响,尽管它对这种金属具有很高的亲和力。在这里,我们研究了双硫仑对乳腺癌细胞的细胞毒性作用,以及其与细胞内和细胞外锌的关系。 MCF-7和BT474癌细胞系在0.01和10μM双硫仑之间产生了惊人的时间依赖性双相细胞毒性反应。双硫仑与低含量锌的共孵育消除了这种效应,表明细胞外锌的可用性显着影响了双硫仑的功效。使用荧光内吞探针和锌染料Fluozin-3进行的活细胞共聚焦显微镜检查显示,双硫仑选择性且迅速地增加了内溶酶体中的锌水平。双硫仑还引起晚期内体和溶酶体的空间混乱,表明它们是该药物的新靶标。通过合成新的双硫仑类似物巩固了双硫仑毒性和离子载体活性之间的这种关系,总的来说,我们证明了双硫仑细胞毒性的新机制,对于将来用作癌症治疗剂具有重要的临床意义。 (C)2015作者。由Elsevier Inc.发布

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