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Diversity of Transgenic Mouse Models for Selective Targeting of Midbrain Dopamine Neurons

机译:选择性靶向中脑多巴胺神经元的转基因小鼠模型的多样性。

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摘要

Ventral tegmental area (VTA) dopamine (DA) neurons have been implicated in reward, aversion, salience, cognition, and several neuropsychiatric disorders. Optogenetic approaches involving transgenic Cre-driver mouse lines provide powerful tools for dissecting DA-specific functions. However, the emerging complexity of VTA circuits requires Cre-driver mouse lines that restrict transgene expression to a precisely defined cell population. Because of recent work reporting that VTA DA neurons projecting to the lateral habenula release GABA, but not DA, we performed an extensive anatomical, molecular, and functional characterization of prominent DA transgenic mouse driver lines. We find that transgenes under control of the tyrosine hydroxylase, but not the dopamine transporter, promoter exhibit dramatic non-DA cell-specific expression patterns within and around VTA nuclei. Our results demonstrate how Cre expression in unintentionally targeted cells in transgenic mouse lines can confound the interpretation of supposedly cell-type-specific experiments. This Matters Arising paper is in response to , published in Neuron. See also the Matters Arising Response paper by , published concurrently with this Matters Arising in Neuron.
机译:腹侧被盖区(VTA)多巴胺(DA)神经元已与奖赏,厌恶,显着性,认知和几种神经精神疾病有关。涉及转基因Cre驱动程序小鼠品系的光遗传学方法为剖析DA特定功能提供了强大的工具。但是,新兴的VTA电路复杂性要求Cre-driver小鼠系将转基因表达限制在精确定义的细胞群体中。由于最近的工作报道了投射到侧ha动脉的VTA DA神经元释放了GABA,但没有释放DA,我们对著名的DA转基因小鼠驱动程序系进行了广泛的解剖,分子和功能表征。我们发现,在酪氨酸羟化酶而不是多巴胺转运蛋白的启动子控制下的转基因启动子在VTA核内和周围展现出戏剧性的非DA细胞特异性表达模式。我们的结果表明,在转基因小鼠品系中无意中靶向细胞中Cre的表达如何混淆推测的特定细胞类型实验的解释。此问题发表是针对,刊登在Neuron上。另请参见由撰写的《问题引起的反应》和《神经元中的问题引起的》同时发表。

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