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黄热病蚊子埃及伊蚊中肠重塑过程中蜕皮激素受体和蜕皮激素诱导转录因子的阶段特异性和细胞特异性表达。

Stage- and cell-specific expression of ecdysone receptors and ecdysone-induced transcription factors during midgut remodeling in the yellow fever mosquito, Aedes aegypti.

作者信息

Parthasarathy R, Palli Subba R

机构信息

Department of Entomology, College of Agriculture, University of Kentucky, Lexington, KY 40546, USA.

出版信息

J Insect Physiol. 2007 Mar;53(3):216-29. doi: 10.1016/j.jinsphys.2006.09.009. Epub 2006 Sep 19.

Abstract

In insects, especially in mosquitoes that are adult blood feeders, midgut remodeling is an important event during metamorphosis. It involves two processes viz., programmed cell death (PCD) of larval cells, and proliferation and differentiation of imaginal cells to form pupal/adult midgut. These processes are regulated by 20-hydroxyecdysone (20E) and juvenile hormone (JH), but the signaling mechanisms, which trigger specific changes remain poorly understood. Here, we report stage- and cell-specific expression of ecydone receptor (EcR), ultraspiracle (USP), broad (Br), E75B and hormone receptor 3 (HR3) during midgut remodeling in Aedes aegypti. In Ae. aegypti both EcR and USP genes code for two isoforms each and the expression of mRNA for these isoforms showed both stage- and cell-specific regulation. In general, EcR-B and USP-A mRNAs were detected during larval stages in larval cells, and EcR-A and USP-B mRNAs were detected during pupal stages in imaginal cells. These data suggest that EcR-B/USP-A heterodimer is important for PCD of larval cells and EcR-A/USP-B heterodimer is important for formation of pupal/adult midgut. Broad Z1 mRNA was detected only in the larval cells suggesting its primary role in PCD. It is likely that E75B and HR3 are probably involved in both PCD and imaginal cell proliferation and differentiation as their mRNAs were expressed in the larval as well as in imaginal cells. Application of JH analog, methoprene, lowered or delayed the expression of all the genes studied. These data suggest that 20E plays a major role in midgut remodeling and coordinates this process through stage- and cell-specific expression of different isoforms of nuclear receptors and transcription factors in the target larval and imaginal cells.

摘要

在昆虫中,尤其是在吸食成虫血液的蚊子中,中肠重塑是变态发育过程中的一个重要事件。它涉及两个过程,即幼虫细胞的程序性细胞死亡(PCD)以及成虫细胞的增殖和分化以形成蛹期/成虫期的中肠。这些过程受20-羟基蜕皮酮(20E)和保幼激素(JH)调控,但引发特定变化的信号传导机制仍知之甚少。在此,我们报告了埃及伊蚊中肠重塑过程中蜕皮酮受体(EcR)、超气门蛋白(USP)、宽型(Br)、E75B和激素受体3(HR3)的阶段特异性和细胞特异性表达。在埃及伊蚊中,EcR和USP基因各自编码两种亚型,这些亚型的mRNA表达呈现出阶段特异性和细胞特异性调控。一般来说,在幼虫阶段的幼虫细胞中检测到EcR-B和USP-A的mRNA,而在蛹期的成虫细胞中检测到EcR-A和USP-B的mRNA。这些数据表明,EcR-B/USP-A异二聚体对幼虫细胞的PCD很重要,而EcR-A/USP-B异二聚体对蛹期/成虫期的中肠形成很重要。仅在幼虫细胞中检测到宽型Z1的mRNA,表明其在PCD中起主要作用。E75B和HR3可能参与了PCD以及成虫细胞的增殖和分化,因为它们的mRNA在幼虫细胞和成虫细胞中均有表达。应用JH类似物烯虫酯可降低或延迟所研究的所有基因的表达。这些数据表明,20E在中肠重塑中起主要作用,并通过靶标幼虫细胞和成虫细胞中核受体和转录因子不同亚型的阶段特异性和细胞特异性表达来协调这一过程。

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