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Broad-Complex在保幼激素信号传导中位于Met的下游发挥作用,以协调原始全变态昆虫的变态发育。

Broad-Complex acts downstream of Met in juvenile hormone signaling to coordinate primitive holometabolan metamorphosis.

作者信息

Konopova Barbora, Jindra Marek

机构信息

Biology Center, Czech Academy of Sciences, Czech Republic.

出版信息

Development. 2008 Feb;135(3):559-68. doi: 10.1242/dev.016097. Epub 2008 Jan 2.

Abstract

Metamorphosis of holometabolous insects, an elaborate change of form between larval, pupal and adult stages, offers an ideal system to study the regulation of morphogenetic processes by hormonal signals. Metamorphosis involves growth and differentiation, tissue remodeling and death, all of which are orchestrated by the morphogenesis-promoting ecdysteroids and the antagonistically acting juvenile hormone (JH), whose presence precludes the metamorphic changes. How target tissues interpret this combinatorial effect of the two hormonal cues is poorly understood, mainly because JH does not prevent larval-pupal transformation in the derived Drosophila model, and because the JH receptor is unknown. We have recently used the red flour beetle Tribolium castaneum to show that JH controls entry to metamorphosis via its putative receptor Methoprene-tolerant (Met). Here, we demonstrate that Met mediates JH effects on the expression of the ecdysteroid-response gene Broad-Complex (BR-C). Using RNAi and a classical mutant, we show that Tribolium BR-C is necessary for differentiation of pupal characters. Furthermore, heterochronic combinations of retarded and accelerated phenotypes caused by impaired BR-C function suggest that besides specifying the pupal fate, BR-C operates as a temporal coordinator of hormonally regulated morphogenetic events across epidermal tissues. Similar results were also obtained when using the lacewing Chrysopa perla (Neuroptera), a member of another holometabolous group with a primitive type of metamorphosis. The tissue coordination role of BR-C may therefore be a part of the Holometabola groundplan.

摘要

全变态昆虫的变态过程,即幼虫、蛹和成虫阶段之间形式上的精细变化,为研究激素信号对形态发生过程的调控提供了一个理想的系统。变态涉及生长与分化、组织重塑与死亡,所有这些过程均由促进形态发生的蜕皮甾类和起拮抗作用的保幼激素(JH)协调,JH的存在会阻止变态变化。目前人们对靶组织如何解读这两种激素信号的组合效应了解甚少,主要原因是在衍生的果蝇模型中JH并不阻止幼虫到蛹的转变,且JH受体尚不明确。我们最近利用赤拟谷盗来表明JH通过其假定的受体耐甲氧普烯(Met)来控制进入变态的过程。在此,我们证明Met介导了JH对蜕皮甾类反应基因Broad-Complex(BR-C)表达的影响。利用RNA干扰和一个经典突变体,我们表明拟谷盗的BR-C对于蛹特征的分化是必需的。此外,由BR-C功能受损导致的发育迟缓与加速表型的异时组合表明,除了决定蛹的命运外,BR-C还作为整个表皮组织中激素调节的形态发生事件的时间协调者发挥作用。当使用草蛉(脉翅目)时也获得了类似结果,草蛉是具有原始变态类型的另一全变态类群的成员。因此,BR-C的组织协调作用可能是全变态类基本模式的一部分。

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