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Targeting an oncogenic kinase/phosphatase signaling network for cancer therapy

机译:靶向致癌激酶/磷酸酶信号网络进行癌症治疗

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摘要

Protein kinases and phosphatases signal by phosphorylation and dephosphorylation to precisely control the activities of their individual and common substrates for a coordinated cellular outcome. In many situations, a kinase/phosphatase complex signals dynamically in time and space through their reciprocal regulations and their cooperative actions on a substrate. This complex may be essential for malignant transformation and progression and can therefore be considered as a target for therapeutic intervention. p38γ is a unique MAPK family member that contains a PDZ motif at its C-terminus and interacts with a PDZ domain-containing protein tyrosine phosphatase PTPH1. This PDZ-coupled binding is required for both PTPH1 dephosphorylation and inactivation of p38γ and for p38γ phosphorylation and activation of PTPH1. Moreover, the p38γ/PTPH1 complex can further regulate their substrates phosphorylation and dephosphorylation, which impacts Ras transformation, malignant growth and progression, and therapeutic response. This review will use the p38γ/PTPH1 signaling network as an example to discuss the potential of targeting the kinase/phosphatase signaling complex for development of novel targeted cancer therapy.
机译:蛋白激酶和磷酸酶通过磷酸化和去磷酸化来发出信号,以精确控制它们各自和共同底物的活性,从而实现协调的细胞结果。在许多情况下,激酶/磷酸酶复合物通过其相互调节及其在底物上的协同作用在时间和空间上动态发出信号。该复合物对于恶性转化和进展可能是必不可少的,因此可以被视为治疗干预的靶标。 p38γ是一个独特的MAPK家族成员,在其C端包含一个PDZ基序,并与包含PDZ域的蛋白酪氨酸磷酸酶PTPH1相互作用。 PDZ偶联需要PTPH1去磷酸化和p38γ失活以及p38γ磷酸化和PTPH1活化。而且,p38γ/ PTPH1复合物可以进一步调节其底物的磷酸化和去磷酸化,从而影响Ras转化,恶性生长和进展以及治疗反应。这篇综述将以p38γ/ PTPH1信号网络为例,讨论靶向激酶/磷酸酶信号复合物开发新型靶向癌症疗法的潜力。

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