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Targeting ATM pathway for therapeutic intervention in cancer

机译:针对ATM途径的癌症治疗干预

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摘要

The Ataxia Telangiectasia Mutated gene encodes the ATM protein, a key element in the DNA damage response (DDR) signalling pathway responsible for maintaining genomic integrity within the cell. The ATM protein belongs to a family of large protein kinases containing the phosphatidylinositol-3 catalytic domain, including ATM, ATR and PI3K. ATM provides the crucial link between DNA damage, cell cycle progression and cell death by first sensing double stranded DNA breaks and subsequently phosphorylating and activating other downstream proteins functioning in DNA damage repair, cell cycle arrest and apoptotic pathways,. Mammalian cells are constantly challenged by genotoxic agents from a variety of sources and therefore require a robust sensing and repair mechanism to maintain DNA integrity or activate alternative cell fate pathways. This review covers the role of ATM in DDR signalling and describes the interaction of the ATM kinase with other proteins in order to fulfil its various functions. Special emphasis is given to how the growing knowledge of the DDR can help identify drug targets for cancer therapy, thus providing a rationale for exploiting the ATM pathway in anticancer drug development. Moreover, we discuss how a network modelling approach can be used to identify and characterise ATM inhibitors and predict their therapeutic potential.
机译:共济失调毛细血管扩张突变基因编码ATM蛋白,ATM蛋白是DNA损伤反应(DDR)信号传导途径中的关键元素,负责维持细胞内的基因组完整性。 ATM蛋白属于包含磷脂酰肌醇3催化域的大蛋白激酶家族,包括ATM,ATR和PI3K。 ATM通过首先检测双链DNA断裂,然后磷酸化和激活在DNA损伤修复,细胞周期停滞和凋亡途径中起作用的其他下游蛋白,在DNA损伤,细胞周期进程和细胞死亡之间提供了至关重要的联系。哺乳动物细胞不断受到来自各种来源的遗传毒性剂的挑战,因此需要强大的传感和修复机制来维持DNA完整性或激活其他细胞命运途径。这篇综述涵盖了ATM在DDR信号传导中的作用,并描述了ATM激酶与其他蛋白质的相互作用,以实现其各种功能。特别强调的是,越来越多的DDR知识如何帮助确定用于癌症治疗的药物靶标,从而为在抗癌药物开发中利用ATM途径提供了理论依据。此外,我们讨论了如何使用网络建模方法来识别和表征ATM抑制剂并预测其治疗潜力。

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