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RNAi screening for kinases and phosphatases identifies FoxO regulators

机译:RNAi筛选激酶和磷酸酶可识别FoxO调节剂

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摘要

Forkhead box class O (FoxO) transcription factors are key regulators of growth, metabolism, life span, and stress resistance. FoxOs integrate signals from different pathways and guide the cellular response to varying energy and stress conditions. FoxOs are modulated by several signaling pathways, e.g., the insulin-TOR signaling pathway and the stress induced JNK signaling pathway. Here, we report a genome wide RNAi screen of kinases and phosphatases aiming to find regulators of dFoxO activity in Dro-sophila S2 cells. By using a combination of transcriptional activity and localization assays we identified several enzymes that modulate dFoxO transcriptional activity, intracellular localization and/or protein stability. Importantly, several currently known dFoxO regulators were found in the screening, confirming the validity of our approach. In addition, several interesting new regulators were identified, including protein kinase C and glycogen synthase kinase 3/J, two proteins with important roles in insulin signaling. Furthermore, several mammalian orthologs of the proteins identified in Drosophila also regulate FOXO activity in mammalian cells. Our results contribute to a comprehensive understanding of FoxO regulatory processes.
机译:O型前叉箱(FoxO)转录因子是生长,代谢,寿命和抗逆性的关键调节剂。 FoxO整合来自不同途径的信号,并指导细胞对变化的能量和压力条件做出反应。 FoxO受几种信号传导途径调节,例如胰岛素-TOR信号传导途径和应激诱导的JNK信号传导途径。在这里,我们报道了激酶和磷酸酶的全基因组RNAi筛选,旨在在果蝇S2细胞中寻找dFoxO活性的调节剂。通过结合使用转录活性和定位分析,我们确定了几种调节dFoxO转录活性,细胞内定位和/或蛋白质稳定性的酶。重要的是,在筛选中发现了几种当前已知的dFoxO调节剂,证实了我们方法的有效性。另外,鉴定了几种有趣的新调节剂,包括蛋白激酶C和糖原合酶激酶3 / J,这两种蛋白在胰岛素信号传导中具有重要作用。此外,在果蝇中鉴定的蛋白质的几种哺乳动物直系同源物也调节哺乳动物细胞中的FOXO活性。我们的结果有助于全面了解FoxO监管流程。

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