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p53介导的细胞代谢间接调控:从发病机制到癌症治疗的发展

p53-Mediated Indirect Regulation on Cellular Metabolism: From the Mechanism of Pathogenesis to the Development of Cancer Therapeutics.

作者信息

Wang Chen-Yun, Chao Chi-Hong

机构信息

Institute of Molecular Medicine and Bioengineering, National Yang Ming Chiao Tung University, Hsinchu, Taiwan.

Center For Intelligent Drug Systems and Smart Bio-devices (IDS2B), National Yang Ming Chiao Tung University, Hsinchu, Taiwan.

出版信息

Front Oncol. 2022 May 30;12:895112. doi: 10.3389/fonc.2022.895112. eCollection 2022.

Abstract

The transcription factor p53 is the most well-characterized tumor suppressor involved in multiple cellular processes, which has expanded to the regulation of metabolism in recent decades. Accumulating evidence reinforces the link between the disturbance of p53-relevant metabolic activities and tumor development. However, a full-fledged understanding of the metabolic roles of p53 and the underlying detailed molecular mechanisms in human normal and cancer cells remain elusive, and persistent endeavor is required to foster the entry of drugs targeting p53 into clinical use. This mini-review summarizes the indirect regulation of cellular metabolism by wild-type p53 as well as mutant p53, in which mechanisms are categorized into three major groups: through modulating downstream transcriptional targets, protein-protein interaction with other transcription factors, and affecting signaling pathways. Indirect mechanisms expand the p53 regulatory networks of cellular metabolism, making p53 a master regulator of metabolism and a key metabolic sensor. Moreover, we provide a brief overview of recent achievements and potential developments in the therapeutic strategies targeting mutant p53, emphasizing synthetic lethal methods targeting mutant p53 with metabolism. Then, we delineate synthetic lethality targeting mutant p53 with its indirect regulation on metabolism, which expands the synthetic lethal networks of mutant p53 and broadens the horizon of developing novel therapeutic strategies for p53 mutated cancers, providing more opportunities for cancer patients with mutant p53. Finally, the limitations and current research gaps in studies of metabolic networks controlled by p53 and challenges of research on p53-mediated indirect regulation on metabolism are further discussed.

摘要

转录因子p53是参与多种细胞过程的特征最为明确的肿瘤抑制因子,近几十年来其作用已扩展至对代谢的调控。越来越多的证据强化了与p53相关的代谢活动紊乱与肿瘤发生之间的联系。然而,对于p53在人类正常细胞和癌细胞中的代谢作用及其潜在的详细分子机制仍缺乏全面了解,需要持续努力以推动靶向p53的药物进入临床应用。本综述总结了野生型p53以及突变型p53对细胞代谢的间接调控,其机制分为三大类:通过调节下游转录靶点、与其他转录因子进行蛋白质-蛋白质相互作用以及影响信号通路。间接机制扩展了p53对细胞代谢的调控网络,使p53成为代谢的主要调节因子和关键的代谢传感器。此外,我们简要概述了靶向突变型p53的治疗策略的最新成果和潜在进展,重点强调了针对突变型p53与代谢的合成致死方法。然后,我们阐述了针对突变型p53及其对代谢的间接调控的合成致死性,这扩展了突变型p53的合成致死网络,拓宽了开发针对p53突变癌症的新型治疗策略的视野,为携带突变型p53的癌症患者提供了更多机会。最后,进一步讨论了p53控制的代谢网络研究中的局限性和当前研究空白以及p53介导的对代谢的间接调控研究面临的挑战。

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