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Effect of Proliferating Cell Nuclear Antigen Ubiquitination and Chromatin Structure on the Dynamic Properties of the Y-family DNA Polymerases

机译:增殖细胞核抗原的泛素化和染色质结构对Y家族DNA聚合酶动力学特性的影响。

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摘要

Y-family DNA polymerases carry out translesion synthesis past damaged DNA. DNA polymerases (pol) η and ι are usually uniformly distributed through the nucleus but accumulate in replication foci during S phase. DNA-damaging treatments result in an increase in S phase cells containing polymerase foci. Using photobleaching techniques, we show that polη is highly mobile in human fibroblasts. Even when localized in replication foci, it is only transiently immobilized. Although ubiquitination of proliferating cell nuclear antigen (PCNA) is not required for the localization of polη in foci, it results in an increased residence time in foci. polι is even more mobile than polη, both when uniformly distributed and when localized in foci. Kinetic modeling suggests that both polη and polι diffuse through the cell but that they are transiently immobilized for ∼150 ms, with a larger proportion of polη than polι immobilized at any time. Treatment of cells with DRAQ5, which results in temporary opening of the chromatin structure, causes a dramatic immobilization of polη but not polι. Our data are consistent with a model in which the polymerases are transiently probing the DNA/chromatin. When DNA is exposed at replication forks, the polymerase residence times increase, and this is further facilitated by the ubiquitination of PCNA.
机译:Y族DNA聚合酶通过受损的DNA进行跨病变合成。 DNA聚合酶(pol)η和η通常在细胞核中均匀分布,但在S期中聚集在复制灶中。 DNA损伤处理导致含有聚合酶灶的S期细胞增加。使用光漂白技术,我们表明poln在人类成纤维细胞中具有很高的移动性。即使位于复制灶中,也只能暂时固定。尽管在病灶中定位poln不需要增殖细胞核抗原(PCNA)的泛素化,但这会导致在病灶中的停留时间增加。无论是均匀分布还是局部聚焦,poli都比poln更具移动性。动力学模型表明,poln和poli均扩散通过细胞,但是它们被瞬时固定约150ms,其中polη比在任何时候固定的poli更大。用DRAQ5处理细胞会导致染色质结构的暂时打开,从而导致极显着的固定化,而不引起极度的固定化。我们的数据与聚合酶瞬时探测DNA /染色质的模型一致。当DNA在复制叉处暴露时,聚合酶的停留时间会增加,而PCNA的泛素化会进一步促进这种情况。

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