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Zeste tunes the timing of ecdysone actions in triggering programmed tissue degeneration in Drosophila

机译:Zeste调节蜕皮激素在果蝇中触发程序性组织变性的时机

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In the pupal stage, the fly body undergoes extensive metamorphic remodeling, in which programmed cell death plays a critical role. We studied two of the constituent processes in this remodeling, salivary gland degeneration and breakdown of the eclosion muscle, which are triggered by an increase and a decrease in the circulating steroid hormone ecdysone at the start and end of metamorphosis, respectively. We found that knockdown of zeste (z), a gene encoding a sequence-specific DNA-binding protein implicated in transvection, in salivary gland cells advances the initiation of their degeneration, whereas z knockdown in neurons delays muscle breakdown. We further showed that knockdown of an ecdysone-inducible gene, E74, retards salivary gland degeneration with little effect on eclosion muscle breakdown. We propose that Z tunes the sensitivity of ecdysone targets to this hormone in order to ensure a high safety margin so that the cell death program will be activated when the ecdysone titer is at a sufficiently high level that is reached only at a defined stage during metamorphosis.
机译:在the期,蝇体经历了广泛的变态重塑,其中程序性细胞死亡起着至关重要的作用。我们研究了这种重塑过程中的两个组成过程,即唾液腺变性和脱落肌的分解,这分别是由蜕变开始和结束时循环类固醇激素蜕皮激素的增加和减少所触发的。我们发现在唾液腺细胞中敲除zeste(z)(一种编码与跨膜相关的序列特异性DNA结合蛋白的基因)的敲击可促进其变性的启动,而在神经元中敲除z的敲除可延迟肌肉衰竭。我们进一步表明,蜕皮激素诱导基因E74的基因敲低可抑制唾液腺变性,而对脊髓垂体肌肉衰竭几乎没有影响。我们建议Z​​调整蜕皮激素靶标对该激素的敏感性,以确保较高的安全裕度,以便当蜕皮激素滴度处于足够高的水平(仅在变态期间的定义阶段达到)时,将激活细胞死亡程序。

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