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通过耐甲氧普烯和广谱复合体之间的遗传相互作用揭示的黑腹果蝇激素信号通路之间的相互作用

Interaction between hormonal signaling pathways in Drosophila melanogaster as revealed by genetic interaction between methoprene-tolerant and broad-complex.

作者信息

Wilson Thomas G, Yerushalmi Yoram, Donnell David M, Restifo Linda L

机构信息

Department of Entomology, Ohio State University, Columbus, OH 43210, USA.

出版信息

Genetics. 2006 Jan;172(1):253-64. doi: 10.1534/genetics.105.046631. Epub 2005 Oct 3.

Abstract

Juvenile hormone (JH) regulates insect development by a poorly understood mechanism. Application of JH agonist insecticides to Drosophila melanogaster during the ecdysone-driven onset of metamorphosis results in lethality and specific morphogenetic defects, some of which resemble those in mutants of the ecdysone-regulated Broad-Complex (BR-C). The Methoprene-tolerant (Met) bHLH-PAS gene mediates JH action, and Met mutations protect against the lethality and defects. To explore relationships among these two genes and JH, double mutants were constructed between Met alleles and alleles of each of the BR-C complementation groups: broad (br), reduced bristles on palpus (rbp), and 2Bc. Defects in viability and oogenesis were consistently more severe in rbp Met or br Met double mutants than would be expected if these genes act independently. Additionally, complementation between BR-C mutant alleles often failed when MET was absent. Patterns of BRC protein accumulation during metamorphosis revealed essentially no difference between wild-type and Met-null individuals. JH agonist treatment did not block accumulation of BRC proteins. We propose that MET and BRC interact to control transcription of one or more downstream effector genes, which can be disrupted either by mutations in Met or BR-C or by application of JH/JH agonist, which alters MET interaction with BRC.

摘要

保幼激素(JH)通过一种尚不清楚的机制调节昆虫发育。在蜕皮激素驱动的变态开始期间,将JH激动剂杀虫剂应用于黑腹果蝇会导致死亡和特定的形态发生缺陷,其中一些缺陷类似于蜕皮激素调节的广谱复合体(BR-C)突变体中的缺陷。耐甲氧普烯(Met)的bHLH-PAS基因介导JH作用,Met突变可防止死亡和缺陷。为了探究这两个基因与JH之间的关系,构建了Met等位基因与BR-C每个互补组(broad,br;触须刚毛减少,rbp;以及2Bc)的等位基因之间的双突变体。与这些基因独立发挥作用时的预期情况相比,rbp Met或br Met双突变体在活力和卵子发生方面的缺陷始终更为严重。此外,当MET不存在时,BR-C突变等位基因之间的互补常常失败。变态期间BRC蛋白积累的模式显示,野生型和Met缺失个体之间基本没有差异。JH激动剂处理并未阻断BRC蛋白的积累。我们提出,MET和BRC相互作用以控制一个或多个下游效应基因的转录,Met或BR-C中的突变或JH/JH激动剂的应用会破坏这种相互作用,而JH/JH激动剂的应用会改变MET与BRC的相互作用。

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