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果蝇EcR-B蜕皮激素受体亚型在幼虫蜕皮和变态发育期间的神经元重塑过程中是必需的。

Drosophila EcR-B ecdysone receptor isoforms are required for larval molting and for neuron remodeling during metamorphosis.

作者信息

Schubiger M, Wade A A, Carney G E, Truman J W, Bender M

机构信息

Department of Zoology, University of Washington, Seattle, WA 98195, USA.

出版信息

Development. 1998 Jun;125(11):2053-62. doi: 10.1242/dev.125.11.2053.

Abstract

During the metamorphic reorganization of the insect central nervous system, the steroid hormone 20-hydroxyecdysone induces a wide spectrum of cellular responses including neuronal proliferation, maturation, cell death and the remodeling of larval neurons into their adult forms. In Drosophila, expression of specific ecdysone receptor (EcR) isoforms has been correlated with particular responses, suggesting that different EcR isoforms may govern distinct steroid-induced responses in these cells. We have used imprecise excision of a P element to create EcR deletion mutants that remove the EcR-B promoter and therefore should lack EcR-B1 and EcR-B2 expression but retain EcR-A expression. Most of these EcR-B mutant animals show defects in larval molting, arresting at the boundaries between the three larval stages, while a smaller percentage of EcR-B mutants survive into the early stages of metamorphosis. Remodeling of larval neurons at metamorphosis begins with the pruning back of larval-specific dendrites and occurs as these cells are expressing high levels of EcR-B1 and little EcR-A. This pruning response is blocked in the EcR-B mutants despite the fact that adult-specific neurons, which normally express only EcR-A, can progress in their development. These observations support the hypothesis that different EcR isoforms control cell-type-specific responses during remodeling of the nervous system at metamorphosis.

摘要

在昆虫中枢神经系统的变态重组过程中,类固醇激素20-羟基蜕皮酮会引发广泛的细胞反应,包括神经元增殖、成熟、细胞死亡以及幼虫神经元重塑为成虫形态。在果蝇中,特定蜕皮激素受体(EcR)亚型的表达与特定反应相关,这表明不同的EcR亚型可能在这些细胞中调控不同的类固醇诱导反应。我们利用P因子的不精确切除来创建EcR缺失突变体,这些突变体去除了EcR-B启动子,因此应该缺乏EcR-B1和EcR-B2的表达,但保留EcR-A的表达。大多数这些EcR-B突变动物在幼虫蜕皮时出现缺陷,停滞在三个幼虫阶段之间的界限处,而较小比例的EcR-B突变体存活到变态的早期阶段。变态过程中幼虫神经元的重塑始于幼虫特异性树突的回缩,并且在这些细胞表达高水平的EcR-B1和低水平的EcR-A时发生。尽管通常仅表达EcR-A的成虫特异性神经元能够正常发育,但EcR-B突变体中的这种回缩反应却被阻断。这些观察结果支持了这样一种假说,即在变态过程中神经系统重塑期间,不同的EcR亚型控制细胞类型特异性反应。

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