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果蝇中环状类固醇生成的正向和反馈调节。

Forward and feedback regulation of cyclic steroid production in Drosophila melanogaster.

作者信息

Parvy Jean-Philippe, Wang Peng, Garrido Damien, Maria Annick, Blais Catherine, Poidevin Mickael, Montagne Jacques

机构信息

CGM, UPR 3404, CNRS, Gif sur Yvette 91190, France Université Pierre et Marie Curie, Paris 75005, France

CGM, UPR 3404, CNRS, Gif sur Yvette 91190, France Université Paris-Sud 11, Orsay 91400, France.

出版信息

Development. 2014 Oct;141(20):3955-65. doi: 10.1242/dev.102020. Epub 2014 Sep 24.

Abstract

In most animals, steroid hormones are crucial regulators of physiology and developmental life transitions. Steroid synthesis depends on extrinsic parameters and autoregulatory processes to fine-tune the dynamics of hormone production. In Drosophila, transient increases of the steroid prohormone ecdysone, produced at each larval stage, are necessary to trigger moulting and metamorphosis. Binding of the active ecdysone (20-hydroxyecdysone) to its receptor (EcR) is followed by the sequential expression of the nuclear receptors E75, DHR3 and βFtz-f1, representing a model for steroid hormone signalling. Here, we have combined genetic and imaging approaches to investigate the precise role of this signalling cascade within theprothoracic gland (PG), where ecdysone synthesis takes place. We show that these receptors operate through an apparent unconventional hierarchy in the PG to control ecdysone biosynthesis. At metamorphosis onset, DHR3 emerges as the downstream component that represses steroidogenic enzymes and requires an early effect of EcR for this repression. To avoid premature repression of steroidogenesis, E75 counteracts DHR3 activity, whereas EcR and βFtz-f1 act early in development through a forward process to moderate DHR3 levels. Our findings suggest that within the steroidogenic tissue, a given 20-hydroxyecdysone peak induces autoregulatory processes to sharpen ecdysone production and to confer competence for ecdysteroid biosynthesis at the next developmental phase, providing novel insights into steroid hormone kinetics.

摘要

在大多数动物中,类固醇激素是生理和发育生命转变的关键调节因子。类固醇合成依赖于外在参数和自动调节过程来微调激素产生的动态。在果蝇中,每个幼虫阶段产生的类固醇前体激素蜕皮激素的短暂增加对于触发蜕皮和变态是必要的。活性蜕皮激素(20-羟基蜕皮激素)与其受体(EcR)结合后,核受体E75、DHR3和βFtz-f1会依次表达,这代表了类固醇激素信号传导的一种模式。在这里,我们结合了遗传学和成像方法来研究这一信号级联在蜕皮激素合成发生的前胸腺(PG)中的精确作用。我们表明,这些受体在PG中通过一种明显非常规的层级结构发挥作用,以控制蜕皮激素的生物合成。在变态开始时,DHR3作为下游成分出现,它抑制类固醇生成酶,并且这种抑制需要EcR的早期作用。为了避免过早抑制类固醇生成,E75会抵消DHR3的活性,而EcR和βFtz-f1在发育早期通过正向过程发挥作用,以调节DHR3的水平。我们的研究结果表明,在类固醇生成组织中,特定的20-羟基蜕皮激素峰值会诱导自动调节过程,以增强蜕皮激素的产生,并赋予下一个发育阶段蜕皮甾体生物合成的能力,这为类固醇激素动力学提供了新的见解。

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