Regulation of Cisplatin cytotoxicity by cu influx transporters.

Metal-Based Drugs Pub Date : 2010-01-01 Epub Date: 2011-01-09 DOI:10.1155/2010/317581
Paolo Abada, Stephen B Howell
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引用次数: 48

Abstract

Platinum drugs are an important class of cancer chemotherapeutics. However, the use of these drugs is limited by the development of resistance during treatment with decreased accumulation being a common mechanism. Both Cu transporters CTR1 and CTR2 influence the uptake and cytotoxicity of cisplatin. Although it is structurally similar to CTR1, CTR2 functions in a manner opposite to that of CTR1 with respect to Pt drug uptake. Whereas knockout of CTR1 reduces Pt drug uptake, knockdown of CTR2 enhances cisplatin uptake and cytotoxicity. CTR2 is subject to transcriptional and posttranscriptional regulation by both Cu and cisplatin; this regulation is partly dependent on the Cu chaperone ATOX1. Insight into the mechanisms by which CTR1 and CTR2 regulate sensitivity to the Pt-containing drugs has served as the basis for novel pharmacologic strategies for improving their efficacy.

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铜内流转运体对顺铂细胞毒性的调控。
铂类药物是一类重要的肿瘤化疗药物。然而,这些药物的使用受到治疗期间耐药性发展的限制,减少积累是一种常见的机制。铜转运体CTR1和CTR2都影响顺铂的摄取和细胞毒性。虽然它在结构上与CTR1相似,但在Pt药物摄取方面,CTR2的功能与CTR1相反。敲除CTR1可减少铂类药物的摄取,而敲除CTR2可增强顺铂的摄取和细胞毒性。CTR2受Cu和顺铂的转录和转录后调控;这种调节部分依赖于Cu伴侣ATOX1。深入了解CTR1和CTR2调节对含pt药物敏感性的机制,为提高其疗效的新药理学策略提供了基础。
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Mutagenic Tests Confirm That New Acetylacetonate Pt(II) Complexes Induce Apoptosis in Cancer Cells Interacting with Nongenomic Biological Targets. Cytotoxic properties of titanocenyl amides on breast cancer cell line mcf-7. Role of glutathione in the regulation of Cisplatin resistance in cancer chemotherapy. Hypersensitivity reactions associated with platinum antineoplastic agents: a systematic review. Regulation of Cisplatin cytotoxicity by cu influx transporters.
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