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Heat shock cognate 70 genes contribute to Drosophila spermatocyte growth progression possibly through the insulin signaling pathway

机译:热休克同源70基因可能通过胰岛素信号通路有助于果蝇精子细胞生长进展

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Drosophila spermatocytes grow up to 25 times their original volume before the onset of male meiosis. Several insulin-like peptides and their cognate receptors (InR) are essential for the cell growth process in Drosophila. Here, we aimed to identify additional signaling pathways and other regulatory factors required for germline cell growth in Drosophila males. Spermatocyte-specific expression of the dominant-negative form of InR inhibits cell growth. Conversely, constitutively active forms of signaling factors downstream of InR suppress growth inhibition. Furthermore, hypomorphic mutations in the target of rapamycin (Tor) inhibit spermatocyte growth. These data indicate that the insulin/TOR pathway is essential for the growth of premeiotic spermatocytes. RNA interference (RNAi) screening for the identification of other novel genes associated with cell growth showed that the silencing of each of the five members of heat shock cognate 70 (Hsc70) genes significantly inhibited the process. Hsc70-silenced spermatocytes showed Akt inhibition downstream of the insulin signaling pathway. Our pleckstrin homology domain- green fluorescent protein (PH-GFP) reporter studies indicated that PI3K remained activated in Hsc70-4-silenced cells, suggesting that the Hsc70-4 protein possibly targets Akt or Pdk1 acting downstream of PI3K. Moreover, each of the Hsc70 proteins showed different subcellular localizations. Hsc70-2 exhibited cytoplasmic colocalization with Akt in spermatocytes before nuclear entry of the kinase during the growth phase. These results indicated the involvement of Hsc70 proteins in the activation of various steps in the insulin signaling pathway, which is essential for spermatocyte growth. Our findings provide insights into the mechanism(s) that enhance signal transduction to stimulate the growth of Drosophila spermatocytes.
机译:在雄性减数分裂开始之前,果蝇精母细胞的体积增长到原来的25倍。几种胰岛素样肽及其同源受体(InR)对果蝇的细胞生长过程至关重要。在这里,我们旨在确定果蝇雄性生殖细胞生长所需的其他信号通路和其他调节因子。InR显性阴性形式的精母细胞特异性表达抑制细胞生长。相反,InR下游的组成性活性信号因子抑制生长抑制。此外,雷帕霉素靶基因的亚型突变抑制了精母细胞的生长。这些数据表明,胰岛素/TOR途径对减数分裂前精母细胞的生长至关重要。RNA干扰(RNAi)筛查用于鉴定与细胞生长相关的其他新基因,结果表明,热休克同源基因70(Hsc70)的五个成员中的每一个的沉默都显著抑制了该过程。Hsc70沉默的精母细胞在胰岛素信号通路下游表现出Akt抑制。我们的pleckstrin同源结构域-绿色荧光蛋白(PH-GFP)报告研究表明,PI3K在Hsc70-4沉默的细胞中保持激活状态,这表明Hsc70-4蛋白可能靶向作用于PI3K下游的Akt或Pdk1。此外,每个Hsc70蛋白都显示出不同的亚细胞定位。Hsc70-2在生长期激酶进入细胞核之前,在精母细胞中表现出与Akt的细胞质共定位。这些结果表明Hsc70蛋白参与了胰岛素信号通路中的各个步骤的激活,这对精母细胞的生长至关重要。我们的发现提供了对增强信号转导以刺激果蝇精母细胞生长的机制的见解。

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