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在斑马鱼中囊胚转换阶段通过转录非依赖机制进行的G2期获得。

G2 acquisition by transcription-independent mechanism at the zebrafish midblastula transition.

作者信息

Dalle Nogare Damian E, Pauerstein Philip T, Lane Mary Ellen

机构信息

Department of Biochemistry and Cell Biology, Rice University, MS-140, PO Box 1892, Houston, Texas 77251-1892, USA.

出版信息

Dev Biol. 2009 Feb 1;326(1):131-42. doi: 10.1016/j.ydbio.2008.11.002. Epub 2008 Nov 14.

Abstract

Following fertilization of many animal embryos, rapid synchronous cleavage divisions give way to longer, asynchronous cell cycles at the midblastula transition (MBT). The cell cycle changes at the MBT, including the addition of gap phases and checkpoint controls, are accompanied by activation of the zygotic genome and the onset of cell motility. Whereas the biochemical changes accompanying the MBT in the vertebrate embryo have been extensively documented, the cellular events are not well understood. We show that cell cycle remodeling during the zebrafish MBT includes the transcription-independent acquisition of a G2 phase that is essential for preventing entry into mitosis before S-phase completion in cycles 11-13. We provide evidence from high-resolution imaging that inhibition of Cdc25a and Cdk1 activity, but not Cdk2 activity, is essential for cell cycle lengthening and asynchrony between cycles 9 and 12. We demonstrate that lengthening is not required for initiation of zygotic transcription. Our results are consistent with findings from Drosophila and Xenopus that indicate the central importance of G2 addition in checkpoint establishment, and point to similar mechanisms governing the MBT in diverse species.

摘要

在许多动物胚胎受精后,快速同步的卵裂分裂在中囊胚转换(MBT)时让位于更长的、异步的细胞周期。MBT时的细胞周期变化,包括间隙期的增加和检查点控制,伴随着合子基因组的激活和细胞运动性的开始。虽然脊椎动物胚胎中伴随MBT的生化变化已有大量记录,但细胞事件尚不清楚。我们表明,斑马鱼MBT期间的细胞周期重塑包括G2期的转录非依赖性获得,这对于防止在第11 - 13轮细胞周期中S期完成之前进入有丝分裂至关重要。我们从高分辨率成像中提供证据表明,抑制Cdc25a和Cdk1活性而非Cdk2活性对于第9轮和第12轮细胞周期之间的细胞周期延长和异步性至关重要。我们证明合子转录的起始不需要延长。我们的结果与果蝇和非洲爪蟾的研究结果一致,这些结果表明添加G2在检查点建立中至关重要,并指出不同物种中控制MBT的类似机制。

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