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用于癌症治疗的ERK通路激动作用:证据、见解及一个靶点发现框架

ERK pathway agonism for cancer therapy: evidence, insights, and a target discovery framework.

作者信息

Timofeev Oleg, Giron Philippe, Lawo Steffen, Pichler Martin, Noeparast Maxim

机构信息

Institute of Molecular Oncology, Member of the German Center for Lung Research (DZL), Philipps University, 35043, Marburg, Germany.

Vrije Universiteit Brussel (VUB), Universitair Ziekenhuis Brussel (UZ Brussel), Clinical Sciences, Research group Genetics, Reproduction and Development, Centre for Medical Genetics, Laarbeeklaan 101, 1090, Brussels, Belgium.

出版信息

NPJ Precis Oncol. 2024 Mar 14;8(1):70. doi: 10.1038/s41698-024-00554-5.

Abstract

At least 40% of human cancers are associated with aberrant ERK pathway activity (ERKp). Inhibitors targeting various effectors within the ERKp have been developed and explored for over two decades. Conversely, a substantial body of evidence suggests that both normal human cells and, notably to a greater extent, cancer cells exhibit susceptibility to hyperactivation of ERKp. However, this vulnerability of cancer cells remains relatively unexplored. In this review, we reexamine the evidence on the selective lethality of highly elevated ERKp activity in human cancer cells of varying backgrounds. We synthesize the insights proposed for harnessing this vulnerability of ERK-associated cancers for therapeutical approaches and contextualize these insights within established pharmacological cancer-targeting models. Moreover, we compile the intriguing preclinical findings of ERK pathway agonism in diverse cancer models. Lastly, we present a conceptual framework for target discovery regarding ERKp agonism, emphasizing the utilization of mutual exclusivity among oncogenes to develop novel targeted therapies for precision oncology.

摘要

至少40%的人类癌症与异常的ERK信号通路活性(ERKp)有关。针对ERKp内各种效应器的抑制剂已被开发和研究了二十多年。相反,大量证据表明,正常人类细胞,尤其是癌细胞,对ERKp的过度激活表现出易感性。然而,癌细胞的这种脆弱性仍相对未被探索。在本综述中,我们重新审视了不同背景的人类癌细胞中ERKp活性高度升高导致选择性致死的证据。我们综合了利用ERK相关癌症的这种脆弱性进行治疗方法的见解,并将这些见解置于既定的药理学癌症靶向模型中。此外,我们汇总了不同癌症模型中ERK信号通路激动作用的有趣临床前研究结果。最后,我们提出了一个关于ERKp激动作用靶点发现的概念框架,强调利用癌基因之间的互斥性来开发用于精准肿瘤学的新型靶向疗法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6a31/10940698/8948193630bd/41698_2024_554_Fig1_HTML.jpg

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