Targeting Wee1-like protein kinase to treat cancer.

Anastasios Stathis, Amit Oza
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引用次数: 39

Abstract

New anticancer agents are needed in order to overcome the resistance of cancer cells to standard chemotherapy. At present, many of the molecular events that drive the malignant transformation and progression have been identified and there is optimism that the development of agents that specifically target such events will improve treatment outcomes. Cancer cells present common alterations in components of pathways that are involved in the normal cell cycle regulation and in mechanisms of DNA damage repair. Wee1-like protein kinase is a tyrosine kinase with a key role as an inhibitory regulator of the G2/M checkpoint that precedes entry into mitosis. Abrogation of this checkpoint through Wee1 inhibition may result in increased antitumor activity of agents that cause DNA damage such as radiation therapy or some cytotoxic agents. This has been confirmed in preclinical studies and results of clinical studies evaluating a Wee1 inhibitor are awaited to establish its activity in combination with chemotherapy. Here we review the role of Wee1 tyrosine kinase in the control of the G2/M checkpoint and the effects of G2/M checkpoint abrogation through Wee1 inhibition. We present results of preclinical studies with Wee1 inhibitors and the results of the first clinical trial recently reported, evaluating MK-1775, a small-molecule inhibitor of Wee1.

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靶向wee1样蛋白激酶治疗癌症。
为了克服癌细胞对标准化疗的耐药性,需要新的抗癌药物。目前,许多驱动恶性转化和进展的分子事件已经被确定,人们乐观地认为,专门针对这些事件的药物的开发将改善治疗结果。癌细胞在参与正常细胞周期调节和DNA损伤修复机制的通路成分中表现出共同的改变。wee1样蛋白激酶是一种酪氨酸激酶,在进入有丝分裂之前作为G2/M检查点的抑制调节剂发挥关键作用。通过抑制Wee1来废除这个检查点可能会导致导致DNA损伤的药物(如放疗或某些细胞毒性药物)的抗肿瘤活性增加。这已经在临床前研究中得到证实,临床研究评估Wee1抑制剂的结果有待于确定其与化疗联合的活性。本文综述了Wee1酪氨酸激酶在控制G2/M检查点中的作用以及通过Wee1抑制消除G2/M检查点的作用。我们介绍了Wee1抑制剂的临床前研究结果和最近报道的第一项临床试验的结果,评估了MK-1775,一种Wee1的小分子抑制剂。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Drug news & perspectives
Drug news & perspectives 医学-药学
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>12 weeks
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Osteopontin. Trends in medicinal chemistry. Molecule of the Month. The significance of GlgE as a new target for tuberculosis. Inhibition of potassium currents as a pharmacologic target for investigation in chronic lymphocytic leukemia.
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