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Hot spots of DNA double-strand breaks in human rDNA units are produced in vivo

机译:人体内rDNA单元中DNA双链断裂的热点在体内产生

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摘要

Endogenous hot spots of DNA double-strand breaks (DSBs) are tightly linked with transcription patterns and cancer genomics>1,2. There are nine hot spots of DSBs located in human rDNA units3–6. Here we describe that the profiles of these hot spots coincide with the profiles of γ-H2AX or H2AX, strongly suggesting a high level of in vivo breakage inside rDNA genes. The data were confirmed by microscopic observation of the largest γ-H2AX foci inside nucleoli in interphase chromosomes. In metaphase chromosomes, we observed that only some portion of rDNA clusters possess γ-H2AX foci and that all γ-H2AX foci co-localize with UBF-1 binding sites, which strongly suggests that only active rDNA units possess the hot spots of DSBs. Both γ-H2AX and UBF-1 are epigenetically inherited and thus indicate the rDNA units that were active in the previous cell cycle. These results have implications for diverse fields, including epigenetics and cancer genomics.
机译:DNA双链断裂(DSB)的内源性热点与转录模式和癌症基因组学紧密相关 > 1,2 。位于人类rDNA单元 3-6 的DSB有9个热点。在这里,我们描述了这些热点的轮廓与γ-H2AX或H2AX的轮廓一致,强烈暗示了rDNA基因内部的高水平体内断裂。通过显微镜观察相间染色体中核仁内部最大的γ-H2AX病灶来证实数据。在中期染色体中,我们观察到只有一部分rDNA簇具有γ-H2AX焦点,并且所有γ-H2AX焦点都与UBF-1结合位点共定位,这强烈表明只有活性rDNA单元才具有DSB的热点。 γ-H2AX和UBF-1都是表观遗传的,因此表明在先前的细胞周期中有活性的rDNA单元。这些结果对包括表观遗传学和癌症基因组学在内的各个领域都有影响。

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