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哺乳动物细胞在细胞周期 G1 期和早期 S 期的生化双链断裂修复模型。

Biochemical DSB-repair model for mammalian cells in G1 and early S phases of the cell cycle.

机构信息

Radiation Biophysics Group, Department of Oncology-Pathology, Karolinska Institute, Stockholm SE171 76, Sweden.

出版信息

Mutat Res. 2013 Aug 30;756(1-2):206-12. doi: 10.1016/j.mrgentox.2013.06.004. Epub 2013 Jun 19.

Abstract

The paper presents a model of double strand breaks (DSB) repair in G1 and early S phases of the cell cycle. The model is based on a plethora of published information on biochemical modification of DSB induced by ionizing radiation. So far, three main DSB repair pathways have been identified, including nonhomologous end-joining (NHEJ), homologous recombination (HR), and microhomology-mediated end-joining (MMEJ). During G1 and early S phases of the cell cycle, NHEJ and MMEJ repair pathways are activated dependent on the type of double strand breaks. Simple DSB are a substrate for NHEJ, while complex DSB and DSB in heterochromatin require further end processing. Repair of all DSB start with NHEJ presynaptic processes, and depending on the type of DSB pursue simple ligation, further end processing prior to ligation, or resection. Using law of mass action the model is translated into a mathematical formalism. The solution of the formalism provides the step by step and overall repair kinetics. The overall repair kinetics are compared with the published experimental measurements. Our calculations are in agreement with the experimental results and show that the complex types of DSBs are repaired with slow repair kinetics. The G1 and early S phase model could be employed to predict the kinetics of DSB repair for damage induced by high LET radiation.

摘要

本文提出了一种在细胞周期 G1 期和早期 S 期的双链断裂(DSB)修复模型。该模型基于大量关于电离辐射诱导的 DSB 生化修饰的已发表信息。迄今为止,已经确定了三种主要的 DSB 修复途径,包括非同源末端连接(NHEJ)、同源重组(HR)和微同源介导的末端连接(MMEJ)。在细胞周期的 G1 期和早期 S 期,NHEJ 和 MMEJ 修复途径依赖于双链断裂的类型而被激活。简单的 DSB 是 NHEJ 的底物,而复杂的 DSB 和异染色质中的 DSB 需要进一步的末端加工。所有 DSB 的修复都始于 NHEJ 的预连接过程,并且根据 DSB 的类型,进行简单的连接、连接前的进一步末端加工或切除。通过质量作用定律,该模型被转化为数学形式。形式主义的解提供了逐步和整体的修复动力学。整体修复动力学与已发表的实验测量进行了比较。我们的计算与实验结果一致,表明复杂类型的 DSB 以缓慢的修复动力学进行修复。G1 期和早期 S 期模型可用于预测高 LET 辐射诱导损伤的 DSB 修复动力学。

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