用铜螯合剂增强抗癌药物顺铂的肿瘤特异性摄取。
Enhancing tumor-specific uptake of the anticancer drug cisplatin with a copper chelator.
机构信息
Helen Diller Family Comprehensive Cancer Center, University of California, San Francisco, San Francisco, CA 94143, USA.
出版信息
Cancer Cell. 2010 Jun 15;17(6):574-83. doi: 10.1016/j.ccr.2010.04.011.
Abstract
Uptake of the anticancer drug cisplatin is mediated by the copper transporter CTR1 in cultured cells. Here we show in human ovarian tumors that low levels of Ctr1 mRNA are associated with poor clinical response to platinum-based therapy. Using a mouse model of human cervical cancer, we demonstrate that combined treatment with a copper chelator and cisplatin increases cisplatin-DNA adduct levels in cancerous but not in normal tissues, impairs angiogenesis, and improves therapeutic efficacy. The copper chelator also enhances the killing of cultured human cervical and ovarian cancer cells with cisplatin. Our results identify the copper transporter as a therapeutic target, which can be manipulated with copper chelating drugs to selectively enhance the benefits of platinum-containing chemotherapeutic agents.
摘要
在培养细胞中,抗癌药物顺铂的摄取是由铜转运蛋白 CTR1 介导的。在这里,我们在人类卵巢肿瘤中表明,低水平的 Ctr1 mRNA 与对铂类治疗的临床反应不良相关。使用人宫颈癌的小鼠模型,我们证明联合使用铜螯合剂和顺铂可增加癌细胞而非正常组织中顺铂-DNA 加合物的水平,损害血管生成,并提高治疗效果。铜螯合剂还增强了顺铂对培养的人宫颈癌和卵巢癌细胞的杀伤作用。我们的结果确定了铜转运蛋白作为治疗靶标,可通过铜螯合药物进行操作,以选择性增强含铂化疗药物的益处。
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