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首页> 外文期刊>Developmental biology >Ecdysone signaling opposes epidermal growth factor signaling in regulating cyst differentiation in the male gonad of Drosophila melanogaster
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Ecdysone signaling opposes epidermal growth factor signaling in regulating cyst differentiation in the male gonad of Drosophila melanogaster

机译:蜕皮激素信号转导与表皮生长因子信号转导调控果蝇雄性腺中的囊肿分化

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The development of stem cell daughters into the differentiated state normally requires a cascade of proliferation and differentiation steps that are typically regulated by external signals. The germline cells of most animals, in specific, are associated with somatic support cells and depend on them for normal development. In the male gonad of Drosophila melanogaster, germline cells are completely enclosed by cytoplasmic extensions of somatic cyst cells, and these cysts form a functional unit. Signaling from the germline to the cyst cells via the Epidermal Growth Factor Receptor (EGFR) is required for germline enclosure and has been proposed to provide a temporal signature promoting early steps of differentiation. A temperature-sensitive allele of the EGFR ligand Spitz (Spi) provides a powerful tool for probing the function of the EGRF pathway in this context and for identifying other pathways regulating cyst differentiation via genetic interaction studies. Using this tool, we show that signaling via the Ecdysone Receptor (EcR), a known regulator of developmental timing during larval and pupal development, opposes EGF signaling in testes. In spi mutant animals, reducing either Ecdysone synthesis or the expression of Ecdysone signal transducers or targets in the cyst cells resulted in a rescue of cyst formation and cyst differentiation. Despite of this striking effect in the spi mutant background and the expression of EcR signaling components within the cyst cells, activity of the EcR pathway appears to be dispensable in a wildtype background. We propose that EcR signaling modulates the effects of EGFR signaling by promoting an undifferentiated state in early stage cyst cells. (C) 2014 Elsevier Inc. All rights reserved.
机译:干细胞子代发育为分化状态通常需要一连串的增殖和分化步骤,这些步骤通常受外部信号调节。具体而言,大多数动物的生殖细胞与体细胞支持细胞相关,并依靠它们正常发育。在果蝇的雄性腺中,生殖细胞完全被体细胞囊肿细胞的细胞质延伸所包围,这些囊肿形成一个功能单元。通过表皮生长因子受体(EGFR)从种系传递信号到囊肿细胞是种系封闭所必需的,并且已被提议提供一个促进早期分化步骤的时间特征。 EGFR配体Spitz(Spi)的温度敏感等位基因为在这种情况下探索EGRF途径的功能以及通过遗传相互作用研究鉴定调节囊肿分化的其他途径提供了强大的工具。使用此工具,我们表明通过蜕皮激素受体(EcR)的信号传递,已知的幼虫和p发育过程中的发育时机调节剂,反对睾丸中的EGF信号传导。在spi突变动物中,减少囊胞中的蜕皮激素合成或蜕皮激素信号转导子或靶标的表达导致囊肿形成和囊肿分化得到挽救。尽管在spi突变体背景中具有惊人的效果,并且在囊肿细胞内表达了EcR信号传导成分,但EcR途径的活性似乎在野生型背景中是必需的。我们提出,EcR信号传导通过促进早期囊肿细胞的未分化状态来调节EGFR信号传导的作用。 (C)2014 Elsevier Inc.保留所有权利。

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