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γ-H2AX结构域中双链断裂的积累引发染色体畸变。

Accumulation of DSBs in gamma-H2AX domains fuel chromosomal aberrations.

作者信息

Scherthan H, Hieber L, Braselmann H, Meineke V, Zitzelsberger H

机构信息

Bundeswehr Institute of Radiobiology, Neuherbergstrasse, 11, D-80937 Munich, Germany.

出版信息

Biochem Biophys Res Commun. 2008 Jul 11;371(4):694-7. doi: 10.1016/j.bbrc.2008.04.127. Epub 2008 May 5.

Abstract

DNA double strand breaks (DSBs) pose a severe hazard to the genome as erroneous rejoining of DSBs can lead to mutation and cancer. Here, we have investigated the correlation between X irradiation-induced gamma-H2AX foci, theoretically induced DSBs, and the minimal number of mis-rejoined DNA breaks (MNB) in irradiated lymphocytes obtained from two healthy humans by painting of the whole chromosome complement by spectral karyotyping. There were less gamma-H2AX foci/dose than theoretically expected, while misrepair, as expressed by MNB/gamma-H2AX focus, was similar at 0.5 and 1Gy but 3.6-fold up at 3Gy. Hence, our results suggest that X-ray-induced gamma-H2AX foci in G0 lymphocyte nuclei contain more than one DSB and that the increasing number of DSBs per gamma-H2AX repair factory lead to an increased rate of misrepair.

摘要

DNA双链断裂(DSB)对基因组构成严重威胁,因为DSB的错误重新连接可导致突变和癌症。在此,我们通过光谱核型分析对整个染色体组进行描绘,研究了两名健康人受X射线照射的淋巴细胞中X射线诱导的γ-H2AX焦点、理论上诱导的DSB与错误重新连接的DNA断裂的最小数量(MNB)之间的相关性。γ-H2AX焦点/剂量低于理论预期,而以MNB/γ-H2AX焦点表示的错配修复在0.5和1Gy时相似,但在3Gy时增加了3.6倍。因此,我们的结果表明,G0淋巴细胞核中X射线诱导的γ-H2AX焦点包含不止一个DSB,并且每个γ-H2AX修复工厂中DSB数量的增加导致错配修复率增加。

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