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果蝇原肠胚形成的转录预模式化。

Transcriptional Pre-patterning of Drosophila Gastrulation.

机构信息

Lewis-Sigler Institute for Integrative Genomics, Princeton University, Princeton, NJ 08544, USA.

Department of Molecular Biology, Princeton University, Princeton, NJ 08544, USA.

出版信息

Curr Biol. 2017 Jan 23;27(2):286-290. doi: 10.1016/j.cub.2016.11.047. Epub 2017 Jan 12.

Abstract

Gastrulation of the Drosophila embryo is one of the most intensively studied morphogenetic processes in animal development [1-4]. Particular efforts have focused on the formation of the ventral furrow, whereby ∼1,000 presumptive mesoderm cells exhibit coordinated apical constrictions that mediate invagination [5, 6]. Apical constriction depends on a Rho GTPase signaling pathway (T48/Fog) that is deployed by the developmental regulatory genes twist and snail [7-10]. It is thought that coordinate mesoderm constriction depends on high levels of myosin along the ventral midline, although the basis for this localization is uncertain. Here, we employ newly developed quantitative imaging methods to visualize the transcriptional dynamics of two key components of the Rho signaling pathway in living embryos, T48 and Fog. Both genes display dorsoventral (DV) gradients of expression due to differential timing of transcription activation. Transcription begins as a narrow stripe of two or three cells along the ventral midline, followed by progressive expansions into more lateral regions. Quantitative image analyses suggest that these temporal gradients produce differential spatial accumulations of t48 and fog mRNAs along the DV axis, similar to the distribution of myosin activity. We therefore propose that the transcriptional dynamics of t48 and fog expression foreshadow the coordinated invagination of the mesoderm at the onset of gastrulation.

摘要

果蝇胚胎的原肠胚形成是动物发育中研究最为深入的形态发生过程之一[1-4]。人们特别关注的是腹沟的形成,大约有 1000 个假定的中胚层细胞表现出协调的顶端收缩,介导了内陷[5,6]。顶端收缩依赖于 Rho GTPase 信号通路(T48/Fog),该信号通路由发育调节基因 twist 和 snail 所部署[7-10]。人们认为,协调的中胚层收缩依赖于沿腹中线的高水平肌球蛋白,但这种定位的基础尚不清楚。在这里,我们采用新开发的定量成像方法,可视化了活胚胎中 Rho 信号通路的两个关键成分 T48 和 Fog 的转录动力学。由于转录激活的时间不同,这两个基因都表现出背腹(DV)梯度表达。转录开始时,在腹中线的两到三个细胞处呈狭窄条纹状,然后逐渐扩展到更外侧的区域。定量图像分析表明,这些时间梯度沿 DV 轴产生了 t48 和 fog mRNA 的不同空间积累,类似于肌球蛋白活性的分布。因此,我们提出 t48 和 fog 表达的转录动力学预示着原肠胚形成开始时中胚层的协调内陷。

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