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p53-Mdm2信号通路:新型抗癌疗法的开发靶点

The p53-Mdm2 pathway: targets for the development of new anticancer therapeutics.

作者信息

Zheleva Daniella I, Lane David P, Fischer Peter M

机构信息

Cyclacel Limited, James Lindsay Place, Dundee, Scotland, UK.

出版信息

Mini Rev Med Chem. 2003 May;3(3):257-70. doi: 10.2174/1389557033488178.

Abstract

The tumour suppressor p53 is at the centre of a network of regulatory pathways that guard over the continued integrity of the living cell and its progeny after exposure to different forms of stress, particularly those capable of inducing DNA damage. Tumour cells very frequently circumvent this control by disabling the function of p53, or other proteins in the p53 network, through mutation. Here we review the different therapeutic strategies that have been adopted to exploit common neoplastic aberrations in the p53 pathways. We emphasise in particular those approaches where modulation with pharmaceutical agents has already shown some promise, including pharmacological rescue of mutant p53, modulation of the protein-protein interaction between p53 and one of its negative regulators, Mdm2, as well as interference with downstream targets.

摘要

肿瘤抑制因子p53处于一个调控通路网络的中心,该网络在细胞暴露于不同形式的应激(尤其是那些能够诱导DNA损伤的应激)后,守护活细胞及其后代的持续完整性。肿瘤细胞经常通过突变使p53或p53网络中的其他蛋白质功能失活,从而规避这种控制。在这里,我们综述了为利用p53通路中常见的肿瘤异常而采用的不同治疗策略。我们特别强调那些用药物进行调节已显示出一些前景的方法,包括对突变型p53的药理学挽救、对p53与其负调节因子之一Mdm2之间蛋白质 - 蛋白质相互作用的调节,以及对下游靶点的干扰。

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