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小鼠神经系统中的条件性基因靶向:对脑功能和疾病的见解。

Conditional gene targeting in the mouse nervous system: Insights into brain function and diseases.

作者信息

Gavériaux-Ruff Claire, Kieffer Brigitte L

机构信息

Institut de Génétique et de Biologie Moléculaire et Cellulaire, CNRS/INSERM/ULP, UMR7104, Illkirch, France.

出版信息

Pharmacol Ther. 2007 Mar;113(3):619-34. doi: 10.1016/j.pharmthera.2006.12.003. Epub 2007 Jan 10.

DOI:10.1016/j.pharmthera.2006.12.003
PMID:17289150
Abstract

Conditional gene knockout represents an extremely powerful approach to study the function of single genes in the nervous system. The Cre-LoxP system is the most advanced technology for spatial and temporal control of genetic inactivation, and there is rapid progress using this methodology in neuroscience research. In this approach, mice with LoxP sites flanking the gene of interest (floxed mice) are bred with transgenic mice expressing Cre recombinase under the control of a selected promoter (Cre mice). This promoter is critical in that it determines the time and site of Cre expression. Cre enzyme, in turn, recombines the floxed gene and produces gene knockout. Here we review Cre mouse lines that have been developed to target either the entire brain, selected brain areas, or specific neuronal populations. We then summarize phenotypic consequences of conditional gene targeting in the brain for more than 40 genes, as reported to date. For many broadly expressed genes, brain-restricted knockout has overcome lethality of conventional knockout (KO) and has highlighted a specific role of the encoded protein in some aspect of brain function. In the case of neural genes, data from null mutants in specific brain sites or neurons has refined our understanding of the role of individual molecules that regulate complex behaviors or synaptic plasticity within neural circuits. Among the many developing functional genomic approaches, conditional gene targeting in the mouse has become an excellent tool to elucidate the function of the approximately 5000 known or unknown genes that operate in the nervous system.

摘要

条件性基因敲除是研究单个基因在神经系统中功能的一种极其强大的方法。Cre-LoxP系统是用于基因失活时空控制的最先进技术,并且在神经科学研究中使用该方法取得了快速进展。在这种方法中,将感兴趣基因两侧带有LoxP位点的小鼠(floxed小鼠)与在选定启动子控制下表达Cre重组酶的转基因小鼠(Cre小鼠)进行杂交。该启动子至关重要,因为它决定了Cre表达的时间和位点。Cre酶反过来会重组floxed基因并产生基因敲除。在这里,我们综述了已开发的针对整个大脑、选定脑区或特定神经元群体的Cre小鼠品系。然后,我们总结了迄今为止报道的大脑中条件性基因靶向作用于40多个基因的表型后果。对于许多广泛表达的基因,脑特异性敲除克服了传统敲除(KO)的致死性,并突出了编码蛋白在脑功能某些方面的特定作用。就神经基因而言,来自特定脑区或神经元中无效突变体的数据完善了我们对调节神经回路中复杂行为或突触可塑性的单个分子作用的理解。在众多正在发展的功能基因组学方法中,小鼠中的条件性基因靶向已成为阐明在神经系统中起作用的大约5000个已知或未知基因功能的出色工具。

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