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3D-structured illumination microscopy reveals clustered DNA double-strand break formation in widespread γH2AX foci after high LET heavy-ion particle radiation

机译:3D结构照明显微镜显示在高LET重离子粒子辐射后在广泛的γH2AX焦点中形成了簇状的DNA双链断裂

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摘要

DNA double-strand breaks (DSBs) induced by ionising radiation are considered the major cause of genotoxic mutations and cell death. While DSBs are dispersed throughout chromatin after X-rays or γ-irradiation, multiple types of DNA damage including DSBs, single-strand breaks and base damage can be generated within 1–2 helical DNA turns, defined as a complex DNA lesion, after high Linear Energy Transfer (LET) particle irradiation. In addition to the formation of complex DNA lesions, recent evidence suggests that multiple DSBs can be closely generated along the tracks of high LET particle irradiation. Herein, by using three dimensional (3D)-structured illumination microscopy, we identified the formation of 3D widespread γH2AX foci after high LET carbon-ion irradiation. The large γH2AX foci in G2-phase cells encompassed multiple foci of replication protein A (RPA), a marker of DSBs undergoing resection during homologous recombination. Furthermore, we demonstrated by 3D analysis that the distance between two individual RPA foci within γH2AX foci was approximately 700 nm. Together, our findings suggest that high LET heavy-ion particles induce clustered DSB formation on a scale of approximately 1 μm3. These closely localised DSBs are considered to be a risk for the formation of chromosomal rearrangement after heavy-ion irradiation.
机译:电离辐射诱导的DNA双链断裂(DSB)被认为是遗传毒性突变和细胞死亡的主要原因。当X射线或γ射线照射后,DSB分散在整个染色质中时,高剂量后1–2螺旋DNA转弯内可形成多种类型的DNA损伤,包括DSB,单链断裂和碱基损伤。线性能量转移(LET)粒子辐照。除了形成复杂的DNA损伤外,最近的证据表明,沿着高LET粒子辐照的轨迹可以紧密产生多个DSB。在这里,通过使用三维(3D)结构的照明显微镜,我们确定了高LET碳离子辐照后3D广泛分布的γH2AX焦点的形成。 G2期细胞中较大的γH2AX灶包括复制蛋白A(RPA)的多个灶,RPA是在同源重组期间进行切除的DSB的标志物。此外,我们通过3D分析证明,γH2AX焦点内两个单独的RPA焦点之间的距离约为700 nm。总之,我们的发现表明,高LET重离子粒子可诱导簇状DSB的形成,规模约为1μm 3 。这些重定位的DSB被认为是重离子辐照后形成染色体重排的风险。

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