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The mechanism of tumour cell death by metal-based anticancer drugs is not only a matter of DNA interactions

机译:金属基抗癌药物导致肿瘤细胞死亡的机制不仅是DNA相互作用的问题

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摘要

Platinum drugs are extensively used in the clinic to treat cancer, often leading to a palliative response rather than a cure. While DNA is considered to be the primary target of platinum drugs, there is no clear relationship between cellular platinum accumulation, DNA platination and Pt-DNA adduct removal, and herein we describe new mechanistic insights of platinum drugs related to the hallmarks of cancer and how they interfere with the tumour microenvironment. We then proceed to describe the properties of other metal drugs, including both non-targeted compounds that do not significantly interact with DNA and targeted compounds that interfere more selectively with specific pathways responsible for tumour growth and invasion. Our analysis of the cancer biology and the selected drugs allows us to propose possible routes for future drug development based on metal scaffolds. (C) 2018 Elsevier B.V. All rights reserved.
机译:铂类药物在临床上广泛用于治疗癌症,通常导致姑息反应而不是治愈。虽然DNA被认为是铂药物的主要靶标,但细胞铂的积累,DNA平台化和Pt-DNA加合物的去除之间没有明确的关系,在此我们描述了与癌症特征有关的铂药物的新机制研究,以及如何它们干扰了肿瘤的微​​环境。然后,我们将继续描述其他金属药物的特性,包括与DNA没有显着相互作用的非靶向化合物和对肿瘤生长和侵袭负责的特定途径更具选择性的干扰的靶向化合​​物。我们对癌症生物学和所选药物的分析使我们能够提出基于金属支架的未来药物开发的可能途径。 (C)2018 Elsevier B.V.保留所有权利。

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