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果蝇蜕皮触发激素受体的剪接异构体具有不同的发育作用。

The Splice Isoforms of the Drosophila Ecdysis Triggering Hormone Receptor Have Developmentally Distinct Roles.

作者信息

Diao Feici, Mena Wilson, Shi Jonathan, Park Dongkook, Diao Fengqiu, Taghert Paul, Ewer John, White Benjamin H

机构信息

Laboratory of Molecular Biology, National Institute of Mental Health, National Institutes of Health, Bethesda, Maryland 20892.

Centro Interdisciplinario de Neurociencia, Universidad de Valparaiso, Playa Ancha, Valparaiso, Chile.

出版信息

Genetics. 2016 Jan;202(1):175-89. doi: 10.1534/genetics.115.182121. Epub 2015 Nov 3.

Abstract

To grow, insects must periodically shed their exoskeletons. This process, called ecdysis, is initiated by the endocrine release of Ecdysis Trigger Hormone (ETH) and has been extensively studied as a model for understanding the hormonal control of behavior. Understanding how ETH regulates ecdysis behavior, however, has been impeded by limited knowledge of the hormone's neuronal targets. An alternatively spliced gene encoding a G-protein-coupled receptor (ETHR) that is activated by ETH has been identified, and several lines of evidence support a role in ecdysis for its A-isoform. The function of a second ETHR isoform (ETHRB) remains unknown. Here we use the recently introduced "Trojan exon" technique to simultaneously mutate the ETHR gene and gain genetic access to the neurons that express its two isoforms. We show that ETHRA and ETHRB are expressed in largely distinct subsets of neurons and that ETHRA- but not ETHRB-expressing neurons are required for ecdysis at all developmental stages. However, both genetic and neuronal manipulations indicate an essential role for ETHRB at pupal and adult, but not larval, ecdysis. We also identify several functionally important subsets of ETHR-expressing neurons including one that coexpresses the peptide Leucokinin and regulates fluid balance to facilitate ecdysis at the pupal stage. The general strategy presented here of using a receptor gene as an entry point for genetic and neuronal manipulations should be useful in establishing patterns of functional connectivity in other hormonally regulated networks.

摘要

为了生长,昆虫必须定期蜕去其外骨骼。这个过程称为蜕皮,由蜕皮触发激素(ETH)的内分泌释放引发,并且作为理解行为的激素控制的模型已被广泛研究。然而,由于对该激素的神经元靶点了解有限,理解ETH如何调节蜕皮行为受到了阻碍。已鉴定出一个编码被ETH激活的G蛋白偶联受体(ETHR)的可变剪接基因,并且有几条证据支持其A异构体在蜕皮中的作用。第二种ETHR异构体(ETHRB)的功能仍然未知。在这里,我们使用最近引入的“特洛伊外显子”技术同时突变ETHR基因,并获得对表达其两种异构体的神经元的遗传通路。我们表明,ETHRA和ETHRB在很大程度上不同的神经元亚群中表达,并且在所有发育阶段,蜕皮都需要表达ETHRA而非ETHRB的神经元。然而,基因和神经元操作都表明ETHRB在蛹期和成虫期而非幼虫期的蜕皮中起重要作用。我们还确定了几个表达ETHR的神经元的功能重要亚群,包括一个共同表达肽促白细胞介素并调节液体平衡以促进蛹期蜕皮的亚群。这里提出的使用受体基因作为遗传和神经元操作切入点的一般策略,应该有助于在其他激素调节网络中建立功能连接模式。

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