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Dithiocarbamate prodrugs activated by prostate specific antigen to target prostate cancer

机译:由前列腺特异性抗原激活的二硫代氨基甲酸酯前药以靶向前列腺癌

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摘要

Disulfiram in conjunction with copper has been shown to be a potent anticancer agent. However, disulfiram's therapeutic potential in prostate cancer is hindered by off-target effects due to its reactive and nucleophilic thiol-containing component, diethyldithiocarbamate (DTC). To minimize undesirable reactivity, we have strategically blocked the thiol moiety in DTC with a cleavable p-aminobenzyl (pAB) group linked to peptide substrates recognized by prostate specific antigen (PSA). Here we report the synthesis and evaluation in cancer cell models of two PSA-activatable prodrugs: HPD (Ac-HSSKLQL-pAB-DTC and RPD (RSSYYSL-pAB-DTC). In vitro exposure to PSA was found to trigger activation of HPD and RPD to release diethyldithiocarbamate, and both prodrugs were found to induce toxicity in prostate cancer cells, with HPD showing the most promising selectivity. With copper supplementation, the IC50 of HPD was 1.4 mu M in PSA-expressing LNCaP cells, and 11 mu M in PC3 cells that do not express PSA. These studies demonstrate the utility of using peptide recognition handles to direct the activity of dithiocarbamate prodrugs for selective cytotoxicity of cancer cells.
机译:二硫氨酸与铜相结合,已被证明是一种有效的抗癌剂。然而,由于其反应性和含亲核硫醇的组分,二乙基硫代氨基甲酸二甲酸二甲酸二甲酸二甲酸二甲酸二甲酸二甲酸二甲酸二甲酸二甲酸二甲酸二甲酸二甲酸二甲酸二甲酸酯(DTC),在前列腺癌中的治疗潜力受前列腺癌的治疗潜力。为了使不希望的反应性最小化,我们将DTC中的硫醇部分策略性地阻断了与通过前列腺特异性抗原(PSA)识别的肽基材连接的可切割的对氨基苄基(PAB)组。在这里,我们报告了两个PSA活化前药的癌细胞模型中的合成和评价:HPD(AC-HSSKLQL-PAB-DTC和RPD(RSSYYSL-PAB-DTC)。发现对PSA的体外接触触发HPD的激活RPD释放二乙基硫代氨基甲酸酯,并发现两种前药诱导前列腺癌细胞中的毒性,HPD显示出最有前途的选择性。随着铜补充,HPD的IC50在表达铜的LNCAP细胞中为1.4μm,11亩PC3不能表达PSA的细胞。这些研究证明了使用肽识别手柄的效用,以指导二硫代氨酸前药的活性用于癌细胞的选择性细胞毒性。

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