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在癌症中靶向 p53:一种蛋白,多个靶点。

Drugging p53 in cancer: one protein, many targets.

机构信息

Department of Molecular Cell Biology, Weizmann Institute of Science, Rehovot, Israel.

出版信息

Nat Rev Drug Discov. 2023 Feb;22(2):127-144. doi: 10.1038/s41573-022-00571-8. Epub 2022 Oct 10.

Abstract

Mutations in the TP53 tumour suppressor gene are very frequent in cancer, and attempts to restore the functionality of p53 in tumours as a therapeutic strategy began decades ago. However, very few of these drug development programmes have reached late-stage clinical trials, and no p53-based therapeutics have been approved in the USA or Europe so far. This is probably because, as a nuclear transcription factor, p53 does not possess typical drug target features and has therefore long been considered undruggable. Nevertheless, several promising approaches towards p53-based therapy have emerged in recent years, including improved versions of earlier strategies and novel approaches to make undruggable targets druggable. Small molecules that can either protect p53 from its negative regulators or restore the functionality of mutant p53 proteins are gaining interest, and drugs tailored to specific types of p53 mutants are emerging. In parallel, there is renewed interest in gene therapy strategies and p53-based immunotherapy approaches. However, major concerns still remain to be addressed. This Review re-evaluates the efforts made towards targeting p53-dysfunctional cancers, and discusses the challenges encountered during clinical development.

摘要

TP53 肿瘤抑制基因的突变在癌症中非常频繁,几十年来,人们一直试图将 p53 的功能恢复到肿瘤中作为一种治疗策略。然而,这些药物开发项目中很少有进入后期临床试验,到目前为止,还没有一种基于 p53 的疗法在美国或欧洲获得批准。这可能是因为,作为一种核转录因子,p53 不具有典型的药物靶点特征,因此长期以来被认为是不可成药的。然而,近年来出现了一些有前途的基于 p53 的治疗方法,包括早期策略的改进版本和使不可成药的靶点可成药的新方法。可以保护 p53 免受其负调节剂影响或恢复突变型 p53 蛋白功能的小分子越来越受到关注,针对特定类型 p53 突变体的药物也正在出现。与此同时,基因治疗策略和基于 p53 的免疫治疗方法也重新受到关注。然而,仍存在一些重大问题有待解决。这篇综述重新评估了针对 p53 功能失调癌症的靶向治疗努力,并讨论了在临床开发过程中遇到的挑战。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e82d/9549847/7af314e1c4b7/41573_2022_571_Fig1_HTML.jpg

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