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Regulatory mechanisms of poly(ADP-ribose) polymerase.

机译:聚(ADP-核糖)聚合酶的调节机制。

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摘要

Here, we describe the latest developments on the mechanistic characterization of poly(ADP-ribose) polymerase (PARP) [EC 2.4.2.30], a DNA-dependent enzyme that catalyzes the synthesis of protein-bound ADP-ribose polymers in eucaryotic chromatin. A detailed kinetic analysis of the automodification reaction of PARP in the presence of nicked dsDNA indicates that protein-poly(ADP-ribosyl)ation probably occurs via a sequential mechanism since enzyme-bound ADP-ribose chains are not reaction intermediates. The multiple enzymatic activities catalyzed by PARP (initiation, elongation, branching and self-modification) are the subject of a very complex regulatory mechanism that may involve allosterism. For instance, while the NAD+ concentration determines the average ADP-ribose polymer size (polymerization reaction), the frequency of DNA strand breaks determines the total number of ADP-ribose chains synthesized (initiation reaction). A general discussion of some of the mechanisms that regulate these multiple catalytic activities of PARP is presented below.
机译:在这里,我们描述了聚(ADP-核糖)聚合酶(PARP)[EC 2.4.2.30]的机制表征的最新进展,这是一种DNA依赖性酶,可催化真核染色质中蛋白质结合的ADP-核糖聚合物的合成。在有缺口的dsDNA存在下对PARP的自动修饰反应进行的详细动力学分析表明,蛋白-聚(ADP-核糖基)化可能是通过顺序机制发生的,因为酶结合的ADP-核糖链不是反应中间体。 PARP催化的多种酶活性(起始,延伸,分支和自我修饰)是涉及变构作用的非常复杂的调控机制的主题。例如,NAD +浓度决定了ADP-核糖聚合物的平均尺寸(聚合反应),而DNA链断裂的频率决定了合成的ADP-核糖链的总数(引发反应)。下面介绍了调节PARP的这些多重催化活性的一些机制的一般性讨论。

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