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未受损的DNA在早期胚胎中传递并增强DNA损伤检查点信号。

Undamaged DNA transmits and enhances DNA damage checkpoint signals in early embryos.

作者信息

Peng Aimin, Lewellyn Andrea L, Maller James L

机构信息

Howard Hughes Medical Institute, Department of Pharmacology, University of Colorado School of Medicine, Aurora, CO 80045, USA.

出版信息

Mol Cell Biol. 2007 Oct;27(19):6852-62. doi: 10.1128/MCB.00195-07. Epub 2007 Jul 30.

Abstract

In Xenopus laevis embryos, the midblastula transition (MBT) at the 12th cell division marks initiation of critical developmental events, including zygotic transcription and the abrupt inclusion of gap phases into the cell cycle. Interestingly, although an ionizing radiation-induced checkpoint response is absent in pre-MBT embryos, introduction of a threshold amount of undamaged plasmid or sperm DNA allows a DNA damage checkpoint response to be activated. We show here that undamaged threshold DNA directly participates in checkpoint signaling, as judged by several dynamic changes, including H2AX phosphorylation, ATM phosphorylation and loading onto chromatin, and Chk1/Chk2 phosphorylation and release from nuclear DNA. These responses on physically separate threshold DNA require gamma-H2AX and are triggered by an ATM-dependent soluble signal initiated by damaged DNA. The signal persists in egg extracts even after damaged DNA is removed from the system, indicating that the absence of damaged DNA is not sufficient to end the checkpoint response. The results identify a novel mechanism by which undamaged DNA enhances checkpoint signaling and provide an example of how the transition to cell cycle checkpoint activation during development is accomplished by maternally programmed increases in the DNA-to-cytoplasm ratio.

摘要

在非洲爪蟾胚胎中,第12次细胞分裂时的中囊胚转换(MBT)标志着关键发育事件的开始,包括合子转录以及细胞周期中突然加入间隙期。有趣的是,尽管在MBT之前的胚胎中不存在电离辐射诱导的检查点反应,但引入阈值量的未受损质粒或精子DNA可激活DNA损伤检查点反应。我们在此表明,未受损的阈值DNA直接参与检查点信号传导,这可通过几种动态变化来判断,包括H2AX磷酸化、ATM磷酸化以及加载到染色质上,还有Chk1/Chk2磷酸化以及从核DNA释放。这些在物理上分离的阈值DNA上的反应需要γ-H2AX,并且由受损DNA引发的ATM依赖性可溶性信号触发。即使从系统中去除受损DNA后,该信号仍在卵提取物中持续存在,这表明没有受损DNA不足以终止检查点反应。这些结果确定了一种新机制,即未受损DNA增强检查点信号传导,并提供了一个例子,说明发育过程中向细胞周期检查点激活的转变是如何通过母源编程增加DNA与细胞质的比例来实现的。

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