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果蝇胚胎后极区域终末间隙基因活性的调控与功能

Control and function of terminal gap gene activity in the posterior pole region of the Drosophila embryo.

作者信息

Brönner G, Jäckle H

机构信息

Institut für Genetik und Mikrobiologie, Universität München, F.R.G.

出版信息

Mech Dev. 1991 Nov;35(3):205-11. doi: 10.1016/0925-4773(91)90019-3.

Abstract

We have studied the genetic requirement for the normal expression of the terminal gap genes huckebein (hkb) and tailless (tll) and their possible function in the posterior pole region of the Drosophila embryo. At the early blastoderm stage, both genes are expressed in largely coextensive expression domains. Our results show that in the posterior region of the embryo both the activation and the control of the spatial limits of tll and hkb expression are critically dependent on torso (tor) activity, which is thought to be a crucial component of a cellular signal transduction pathway provided by the terminal maternal system. Furthermore, the spatial control of hkb and tll expression does not require mutual interactions among each other, nor does it require regulatory input from other gap genes which are essential for the establishment of segmentation in the trunk region of the embryo ("central gap genes"). Therefore, the terminal gap genes have unique regulatory features which are distinct from the central gap genes. In the absence of terminal gap gene activities, as in hkb and tll mutant embryos, the expression domains of the central gap genes expand posteriorly, indicating that the terminal gap gene activities prevent central gap gene expression in the posterior pole region of the wildtype embryo. This, in turn, suggests that the terminal gap gene activities prevent metamerization by repression of central gap genes, thereby distinguishing the segmented trunk from the nonsegmented tail region of the embryo.

摘要

我们研究了末端间隙基因驼背(hkb)和无尾(tll)正常表达的遗传需求及其在果蝇胚胎后极区域可能的功能。在早期胚盘阶段,这两个基因在很大程度上共表达于同一表达区域。我们的结果表明,在胚胎的后部区域,tll和hkb表达的激活以及空间界限的控制都严重依赖于躯干(tor)活性,而躯干活性被认为是末端母体系统提供的细胞信号转导途径的关键组成部分。此外,hkb和tll表达的空间控制既不需要它们彼此之间的相互作用,也不需要来自其他间隙基因的调控输入,而这些间隙基因对于胚胎躯干区域(“中央间隙基因”)的体节形成至关重要。因此,末端间隙基因具有与中央间隙基因不同的独特调控特征。在缺乏末端间隙基因活性的情况下,如在hkb和tll突变胚胎中,中央间隙基因的表达区域向后扩展,这表明末端间隙基因活性可防止野生型胚胎后极区域出现中央间隙基因表达。反过来,这表明末端间隙基因活性通过抑制中央间隙基因来防止分节化,从而将胚胎的分节躯干与不分节的尾部区域区分开来。

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