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观察纹状体信号中的血液酒精浓度:新转基因小鼠的细胞特异性分析。

Looking BAC at striatal signaling: cell-specific analysis in new transgenic mice.

作者信息

Valjent Emmanuel, Bertran-Gonzalez Jesus, Hervé Denis, Fisone Gilberto, Girault Jean-Antoine

机构信息

Inserm, UMR-S 839, 75005 Paris, France.

出版信息

Trends Neurosci. 2009 Oct;32(10):538-47. doi: 10.1016/j.tins.2009.06.005. Epub 2009 Sep 16.

Abstract

Understanding how molecular signaling pathways participate in behavioral responses requires determining precisely in which neuronal populations they are activated. The recent development of bacterial artificial chromosome (BAC) transgenic mice expressing a variety of reporters, epitope tagged-proteins or Cre recombinase driven by specific promoters, is a significant step forward in this direction. These mice help overcome the limitations of traditional approaches that examine an average of signaling events occurring in mixed populations of cells. Here, we review how recent studies using such tools have revisited the regulation of striatal signaling pathways, demonstrating the striking segregation between neurons expressing dopamine D1 and D2 receptors and significantly extending our overall knowledge of striatal neurons. Thus, BAC transgenic mice are changing the way to conceive experiments and provide an opportunity to fill the gaps between molecular and systems neurosciences.

摘要

要理解分子信号通路如何参与行为反应,就需要精确确定它们在哪些神经元群体中被激活。最近,通过细菌人工染色体(BAC)转基因小鼠的开发,这些小鼠能够表达由特定启动子驱动的各种报告基因、表位标记蛋白或Cre重组酶,这在这个方向上迈出了重要的一步。这些小鼠有助于克服传统方法的局限性,传统方法只能检测混合细胞群体中发生的信号事件的平均值。在这里,我们回顾了最近使用这些工具的研究如何重新审视纹状体信号通路的调节,证明了表达多巴胺D1和D2受体的神经元之间存在明显的分离,并显著扩展了我们对纹状体神经元的整体认识。因此,BAC转基因小鼠正在改变实验构思的方式,并为填补分子神经科学和系统神经科学之间的空白提供了机会。

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