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生成 DAT-P2A-Flpo 小鼠品系,用于多巴胺神经元亚群的基因靶向。

Generation of a DAT-P2A-Flpo mouse line for intersectional genetic targeting of dopamine neuron subpopulations.

机构信息

Department of Molecular and Cell Biology, University of California, Berkeley, Berkeley, CA 94720, USA.

Helen Wills Neuroscience Institute, University of California, Berkeley, Berkeley, CA 94720, USA.

出版信息

Cell Rep. 2021 May 11;35(6):109123. doi: 10.1016/j.celrep.2021.109123.

Abstract

Dopaminergic projections exert widespread influence over multiple brain regions and modulate various behaviors including movement, reward learning, and motivation. It is increasingly appreciated that dopamine neurons are heterogeneous in their gene expression, circuitry, physiology, and function. Current approaches to target dopamine neurons are largely based on single gene drivers, which either label all dopamine neurons or mark a subset but concurrently label non-dopaminergic neurons. Here, we establish a mouse line with Flpo recombinase expressed from the endogenous Slc6a3 (dopamine active transporter [DAT]) locus. DAT-P2A-Flpo mice can be used together with Cre-expressing mouse lines to efficiently and selectively label dopaminergic subpopulations using Cre/Flp-dependent intersectional strategies. We demonstrate the utility of this approach by generating DAT-P2A-Flpo;NEX-Cre mice that specifically label Neurod6-expressing dopamine neurons, which project to the nucleus accumbens medial shell. DAT-P2A-Flpo mice add to a growing toolbox of genetic resources that will help parse the diverse functions mediated by dopaminergic circuits.

摘要

多巴胺能投射对多个脑区产生广泛影响,并调节多种行为,包括运动、奖励学习和动机。人们越来越认识到,多巴胺神经元在基因表达、回路、生理学和功能上存在异质性。目前针对多巴胺神经元的方法主要基于单一基因驱动,这些驱动要么标记所有多巴胺神经元,要么标记一部分但同时标记非多巴胺神经元。在这里,我们建立了一种在 Slc6a3(多巴胺转运蛋白 [DAT])基因座表达 Flpo 重组酶的小鼠系。DAT-P2A-Flpo 小鼠可与表达 Cre 的小鼠系一起使用,通过 Cre/Flp 依赖性的交叉策略,高效且选择性地标记多巴胺能亚群。我们通过生成特异性标记投射到伏隔核内侧壳的 Neurod6 表达多巴胺神经元的 DAT-P2A-Flpo;NEX-Cre 小鼠证明了这种方法的实用性。DAT-P2A-Flpo 小鼠增加了一个不断增长的遗传资源工具箱,这将有助于解析多巴胺回路介导的不同功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a089/8240967/dbc4a5e6ff3a/nihms-1709018-f0002.jpg

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