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PARP-1 activation in the ERK signaling pathway.

机译:ERK信号通路中的PARP-1激活。

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摘要

PARP-1 is a highly conserved DNA-binding protein, the most abundant member of the polyADP-ribose polymerases (PARP) family, which catalyzes post-translational modification of proteins by polyADP-ribosylation. This modification affects protein-protein and protein-DNA interactions. Binding of PARP-1 to breakages in damaged DNA causes its activation and auto-polyADP-ribosylation in a process that is pivotal for DNA repair. Our recent findings outlined an alternative mechanism of PARP-1 activation via a direct interaction with phosphorylated ERK2 (externally regulated kinase), which is unrelated to DNA damage and does not involve PARP-1 binding to DNA. Furthermore, ERK2-induced PARP-1 activation dramatically amplifies ERK-signals, enhancing ERK-induced phosphorylation of the transcription factor Elk1 and enhancing core histone acetylation and expression of the Elk1 target gene, c-fos. Thus, PARP-1 activation in the ERK signaling pathway mediates epigenetic mechanisms promoting growth, proliferation and differentiation regulated by the Raf-MEK-ERK phosphorylation cascade.
机译:PARP-1是高度保守的DNA结合蛋白,是polyADP-核糖聚合酶(PARP)家族中最丰富的成员,它通过polyADP-核糖基化催化蛋白质的翻译后修饰。这种修饰影响蛋白质-蛋白质和蛋白质-DNA相互作用。 PARP-1与受损DNA断裂的结合会导致其活化和自动polyADP核糖基化,这一过程对于DNA修复至关重要。我们最近的发现概述了通过与磷酸化ERK2(外部调节的激酶)直接相互作用而激活PARP-1的另一种机制,该机制与DNA损伤无关,并且不涉及PARP-1与DNA的结合。此外,ERK2诱导的PARP-1活化可显着放大ERK信号,增强ERK诱导的转录因子Elk1的磷酸化,并增强核心组蛋白乙酰化和Elk1目标基因c-fos的表达。因此,ERP信号通路中的PARP-1激活介导了表观遗传机制,促进了Raf-MEK-ERK磷酸化级联调节的生长,增殖和分化。

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