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Ecdysone-dependent and ecdysone-independent programmed cell death in the developing optic lobe of Drosophila

机译:果蝇发育中的视神经叶中的蜕皮激素依赖性和蜕皮激素依赖性程序性细胞死亡

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The adult optic lobe of Drosophila develops from the primordium during metamorphosis from mid-3rd larval stage to adult. Many cells die during development of the optic lobe with a peak of the number of dying cells at 24. h after puparium formation (h APF). Dying cells were observed in spatio-temporal specific clusters. Here, we analyzed the function of a component of the insect steroid hormone receptor, EcR, in this cell death. We examined expression patterns of two EcR isoforms, EcR-A and EcR-B1, in the optic lobe. Expression of each isoform altered during development in isoform-specific manner. EcR-B1 was not expressed in optic lobe neurons from 0 to 6. h APF, but was expressed between 9 and 48. h APF and then disappeared by 60. h APF. In each cortex, its expression was stronger in older glia-ensheathed neurons than in younger ones. EcR-B1 was also expressed in some types of glia. EcR-A was expressed in optic lobe neurons and many types of glia from 0 to 60. h APF in a different pattern from EcR-B1. Then, we genetically analyzed EcR function in the optic lobe cell death. At 0. h APF, the optic lobe cell death was independent of any EcR isoforms. In contrast, EcR-B1 was required for most optic lobe cell death after 24. h APF. It was suggested that cell death cell-autonomously required EcR-B1 expressed after puparium formation. ΒFTZ-F1 was also involved in cell death in many dying-cell clusters, but not in some of them at 24. h APF. Altogether, the optic lobe cell death occurred in ecdysone-independent manner at prepupal stage and ecdysone-dependent manner after 24. h APF. The acquisition of ecdysone-dependence was not directly correlated with the initiation or increase of EcR-B1 expression.
机译:果蝇的成人视神经叶在从第3幼体中期到成虫的变态期间从原基发育。许多细胞在视神经的发育过程中死亡,在形成后24小时(h APF),死亡细胞的数量达到峰值。在时空特定簇中观察到死亡细胞。在这里,我们分析了昆虫类固醇激素受体EcR在此细胞死亡中的功能。我们检查了视泡中两种EcR亚型,EcR-A和EcR-B1的表达模式。每个异构体的表达在发育过程中以异构体特异性方式发生变化。 EcR-B1在0至6 h APF中未在视神经元中表达,但在9至48 h APF中表达,然后在60 h APF中消失。在每个皮层中,其在胶质细胞增多的老年神经元中的表达均强于年轻的神经元。 EcR-B1在某些类型的神经胶质细胞中也有表达。 EcR-A在0至60 h APF的视神经元和多种神经胶质细胞中表达,其模式与EcR-B1不同。然后,我们遗传分析了EcR在视神经细胞死亡中的功能。在0. h APF时,视神经细胞死亡与任何EcR亚型无关。相反,在APF 24小时后,大多数视神经细胞死亡都需要EcR-B1。有人提出,细胞死亡需要在形成后自动表达EcR-B1。 ΒFTZ-F1也参与了许多垂死细胞簇的细胞死亡,但在APF 24 h时并未参与其中的一些。总的来说,视神经细胞死亡发生在pu前阶段,与蜕皮激素无关,而在24 h APF后则与蜕皮激素无关。蜕皮激素依赖性的获得与EcR-B1表达的启动或增加没有直接关系。

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