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首页> 外文期刊>Metabolism: Clinical and Experimental >Pharmacological concentrations of irisin increase cell proliferation without influencing markers of neurite outgrowth and synaptogenesis in mouse H19-7 hippocampal cell lines
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Pharmacological concentrations of irisin increase cell proliferation without influencing markers of neurite outgrowth and synaptogenesis in mouse H19-7 hippocampal cell lines

机译:鸢尾素的药理浓度可增加细胞增殖,而不会影响小鼠H19-7海马细胞系中神经突生长和突触形成的标志

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摘要

Aims/Hypothesis Irisin is a novel, myocyte secreted, hormone that has been proposed to mediate the beneficial effects of exercise on metabolism. Irisin is expressed, at lower levels, in human brains and knock-down of the precursor of irisin, FNDC5, decreases neural differentiation of mouse embryonic stem cells. No previous studies have evaluated whether irisin may directly regulate hippocampal neurogenesis in mouse hippocampal neuronal (HN) cells. Methods Hippocampal neurogenesis and irisin signaling were studied in vitro using mouse H19-7 HN cell lines. Results We observed that cell proliferation is regulated by irisin in a dose-dependent manner in mouse H19-7 HN cells. Specifically, physiological concentrations of irisin, 5 to 10 nmol/L, had no effect on cell proliferation when compared to control. By contrast, pharmacological concentrations of irisin, 50 to 100 nmol/L, increased cell proliferation when compared to control. Similar to these results regarding irisin's effects on cell proliferation, we also observed that only pharmacological concentrations of irisin increased STAT3, but not AMPK and/or ERK, activation. Finally, we observed that irisin did not activate either microtubule-associated protein 2, a specific neurite outgrowth marker, or Synapsin, a specific synaptogenesis marker in mouse H19-7 HN cells. Conclusions/Interpretations Our data suggest that irisin, in pharmacological concentrations, increases cell proliferation in mouse H19-7 HN cells via STAT3, but not AMPK and/or ERK, signaling pathways. By contrast, neither physiological nor pharmacological concentrations of irisin alter markers of hippocampal neurogenesis in mouse H19-7 HN cell lines.
机译:目的/假设Irisin是一种新型的,分泌肌细胞的激素,已被提出可调节运动对新陈代谢的有益作用。鸢尾素在人脑中以较低的水平表达,而鸢尾素前体FNDC5的敲低降低了小鼠胚胎干细胞的神经分化。以前没有研究评估虹膜素是否可以直接调节小鼠海马神经元(HN)细胞中的海马神经发生。方法采用小鼠H19-7 HN细胞株体外研究海马神经发生和虹膜信号转导。结果我们观察到,虹膜素在小鼠H19-7 HN细胞中以剂量依赖的方式调节细胞增殖。具体而言,与对照相比,生理浓度的鸢尾素5至10 nmol / L对细胞增殖没有影响。相比之下,与对照相比,虹膜素的药理浓度为50至100 nmol / L,可增加细胞增殖。与关于虹膜素对细胞增殖的影响的这些结果相似,我们还观察到只有虹膜素的药理浓度会增加STAT3的激活,而不是AMPK和/或ERK的激活。最后,我们观察到虹膜素未激活小鼠H19-7 HN细胞中的微管相关蛋白2(特定的神经突增生标记)或Synapsin(特定的突触形成标记)。结论/解释我们的数据表明,在药理学浓度上,虹膜素可通过STAT3而非AMPK和/或ERK信号通路增加小鼠H19-7 HN细胞的细胞增殖。相比之下,在小鼠H19-7 HN细胞系中,虹膜素的生理或药理学浓度均未改变海马神经发生的标志物。

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