Inhibiting the Extracellular Signal-regulated Kinase 1/2 (ERK1/2) Cascade in Cancer and the Heart: for Better or Worse, in Sickness and Health?

Angela Clerk
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Abstract

Review Inhibiting the Extracellular Signal-regulated Kinase 1/2 (ERK1/2) Cascade in Cancer and the Heart: for Better or Worse, in Sickness and Health? Angela Clerk *, Shona U Amadi, Samuel J Smith, and Peter H Sugden School of Biological Sciences, University of Reading, Reading RG6 6AS, UK * Correspondence: a.clerk@reading.ac.uk   Received: 3 April 2024; Revised: 27 April 2024; Accepted: 29 April 2024; Published: 23 May 2024   Abstract: The extracellular signal-regulated kinases 1 and 2 (ERK1/2) are the prototypic mitogen-activated protein kinases, first discovered and investigated in the context of cell division and their role in cancer. ERK1/2 are phosphorylated and activated by upstream kinases, MEK1/2 (also known as MKK1/2) that are in turn phosphorylated and activated by RAF kinases (RAF1, BRAF, ARAF), these being activated by small G proteins of the RAS family (HRAS, KRAS, NRAS). The oncogenic nature of the pathway has resulted in the generation of highly specific inhibitors that are successfully used to treat cancer, particularly melanoma. Those in clinical use currently inhibit some isoforms of RAS, RAF kinases and MEK1/2, with additional inhibitors of these kinases in clinical trials. New drugs are now entering the clinic to inhibit ERK1/2 themselves. The ERK1/2 cascade is also important in the heart. It promotes cardiomyocyte hypertrophy and cardioprotection to counter pathophysiological stresses, and plays a significant role in enhancing cardiac fibrosis with detrimental consequences for cardiac function. Here, we summarise the role of ERK1/2 signalling in cancer and the heart, we outline the development of ERK1/2 cascade inhibitors for cancer providing information on those that are approved as cancer treatments and those which are in clinical trials, and we discuss the known and predicted consequences of these ERK1/2 cascade inhibitors for the heart. Integral with this, we consider whether these drugs are necessarily detrimental to the heart or if/when they may be repurposed to prevent or treat heart failure.
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抑制癌症和心脏中的细胞外信号调节激酶 1/2(ERK1/2)级联:是好是坏?
回顾抑制癌症和心脏中的细胞外信号调节激酶 1/2(ERK1/2)级联:疾病和健康中的好坏?Angela Clerk *、Shona U Amadi、Samuel J Smith 和 Peter H SugdenSchool of Biological Sciences, University of Reading, Reading RG6 6AS, UK* Correspondence: a.clerk@reading.ac.uk Received:摘要:细胞外信号调节激酶 1 和 2(ERK1/2)是丝裂原活化蛋白激酶的原型,最早是在细胞分裂及其在癌症中的作用的背景下被发现和研究的。ERK1/2被上游激酶MEK1/2(又称MKK1/2)磷酸化和激活,MEK1/2又被RAF激酶(RAF1、BRAF、ARAF)磷酸化和激活,这些激酶又被RAS家族的小G蛋白(HRAS、KRAS、NRAS)激活。该通路的致癌特性催生了高度特异性的抑制剂,这些抑制剂被成功用于治疗癌症,尤其是黑色素瘤。目前临床上使用的抑制剂可抑制 RAS、RAF 激酶和 MEK1/2 的某些异构体,还有更多这些激酶的抑制剂正在临床试验中。抑制 ERK1/2 本身的新药正在进入临床。ERK1/2 级联在心脏中也很重要。它促进心肌细胞肥大和心脏保护,以对抗病理生理压力,并在促进心脏纤维化方面发挥重要作用,对心脏功能造成有害影响。在此,我们总结了 ERK1/2 信号在癌症和心脏中的作用,概述了 ERK1/2 级联抑制剂在癌症治疗中的发展情况,提供了已被批准为癌症治疗药物和正在进行临床试验的药物的信息,并讨论了这些 ERK1/2 级联抑制剂对心脏的已知和预测后果。与此同时,我们还考虑了这些药物是否一定会对心脏造成损害,或者是否/何时可以将其重新用于预防或治疗心衰。
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