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The cAMP response element binding protein (CREB) as an integrative HUB selector in metazoans: Clues from the hydra model system

机译:cAMP反应元件结合蛋白(CREB)作为后生动物中的整合HUB选择器:来自hydra模型系统的线索

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In eukaryotic cells, a multiplicity of extra-cellular signals can activate a unique signal transduction system that at the nuclear level will turn on a variety of target genes, eliciting thus diverse responses adapted to the initial signal. How distinct signals can converge on a unique signalling pathway that will nevertheless produce signal-specific responses provides a theoretical paradox that can be traced back early in evolution. In bilaterians, the CREB pathway connects diverse extra-cellular signals via cytoplasmic kinases to the CREB transcription factor and the CBP co-activator, regulating according to the context, cell survival, cell proliferation, cell differentiation, pro-apoptosis, long-term memory, hence achieving a “hub” function for cellular and developmental processes. In hydra, the CREB pathway is highly conserved and activated during early head regeneration through RSK-dependent CREB phosphorylation. We show here that the CREB transcription factor and the RSK kinase are co-expressed in all three hydra cell lineages including dividing interstitial stem cells, proliferating nematoblasts, proliferating spermatogonia and spermatocytes, differentiating and mature neurons as well as ectodermal and endodermal myoepithelial cells. In addition, CREB gene expression is specifically up-regulated during early regeneration and early budding. When the CREB function was chemically prevented, the early post-amputation induction of the HyBraI gene was no longer observed and head regeneration was stacked. Thus, in hydra, the CREB pathway appears already involved in multiple tasks, such as reactivation of developmental programs in an adult context, self-renewal of stem cells, proliferation of progenitors and neurogenesis. Consequently, the hub function played by the CREB pathway was established early in animal evolution and might have contributed to the formation of an efficient oral pole through the integration of the neurogenic and patterning functions.
机译:在真核细胞中,多种细胞外信号可以激活独特的信号转导系统,该系统在核水平上会开启各种靶基因,从而引发适应于初始信号的多种反应。不同信号如何在唯一的信号通路上汇聚,但仍会产生信号特定的响应,这提供了一种理论悖论,可以追溯到进化的早期。在双侧人中,CREB途径通过细胞质激酶将各种细胞外信号连接至CREB转录因子和CBP辅助激活因子,并根据环境,细胞存活,细胞增殖,细胞分化,促凋亡,长期记忆进行调节从而实现了细胞和发育过程的“集线器”功能。在九头蛇中,CREB途径在早期头部再生过程中通过RSK依赖性CREB磷酸化得到高度保守和激活。我们在这里显示出CREB转录因子和RSK激酶在所有三个hydra细胞谱系中共表达,包括分裂间质干细胞,增殖的成核细胞,增殖的精原细胞和精母细胞,分化和成熟的神经元以及外胚层和内胚层上皮细胞。另外,在早期再生和早期出芽期间,CREB基因表达特别上调。当化学预防CREB功能时,不再观察到HyBraI基因在早期截肢后的诱导,并且头再生被堆叠。因此,在水肿中,CREB途径似乎已经参与了多个任务,例如在成人环境下重新激活发育程序,干细胞自我更新,祖细胞增殖和神经发生。因此,CREB途径发挥的枢纽功能在动物进化的早期就已经确立,并且可能通过整合神经原性和模式功能而有助于形成有效的口腔极。

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