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使用转基因试剂定义 POMC 神经元:瞬时 Pomc 表达对不同未成熟神经元群体的影响。

Defining POMC neurons using transgenic reagents: impact of transient Pomc expression in diverse immature neuronal populations.

机构信息

Institute of Human Nutrition, Columbia University, New York, New York 10032, USA.

出版信息

Endocrinology. 2012 Mar;153(3):1219-31. doi: 10.1210/en.2011-1665. Epub 2011 Dec 13.

Abstract

Melanocortin signaling plays a central role in the regulation of phenotypes related to body weight and energy homeostasis. To specifically target and study the function of proopiomelanocortin (POMC) neurons, Pomc promoter elements have been utilized to generate reporter and Cre recombinase transgenic reagents. Across gestation, we find that Pomc is dynamically expressed in many sites in the developing mouse forebrain, midbrain, hindbrain, spinal cord, and retina. Although Pomc expression in most embryonic brain regions is transient, it is sufficient to direct Cre-mediated recombination of floxed alleles. We visualize the populations affected by this transgene by crossing Pomc-Cre mice to ROSA reporter strains and identify 62 sites of recombination throughout the adult brain, including several nuclei implicated in energy homeostasis regulation. To compare the relationship between acute Pomc promoter activity and Pomc-Cre-mediated recombination at the single cell level, we crossed Pomc-enhanced green fluorescent protein (eGFP) and Pomc-Cre;ROSA-tdTomato lines. We detect the highest concentration of Pomc-eGFP+ cells in the arcuate nucleus of the hypothalamus and dentate gyrus but also observe smaller populations of labeled cells in the nucleus of the solitary tract, periventricular zone of the third ventricle, and cerebellum. Consistent with the dynamic nature of Pomc expression in the embryo, the vast majority of neurons marked with the tdTomato reporter do not express eGFP in the adult. Thus, recombination in off-target sites could contribute to physiological phenotypes using Pomc-Cre transgenics. For example, we find that approximately 83% of the cells in the arcuate nucleus of the hypothalamus immunoreactive for leptin-induced phosphorylated signal transducer and activator of transcription 3 are marked with Pomc-Cre;ROSA-tdTomato; only 13% of these are eGFP+ POMC neurons.

摘要

黑皮质素信号在调节与体重和能量平衡相关的表型方面发挥着核心作用。为了专门针对和研究前阿黑皮素原(POMC)神经元的功能,利用 Pomc 启动子元件生成了报告基因和 Cre 重组酶转基因试剂。在整个妊娠期,我们发现 Pomc 在发育中的小鼠前脑、中脑、后脑、脊髓和视网膜的许多部位都有动态表达。尽管大多数胚胎大脑区域的 Pomc 表达是短暂的,但足以指导 floxed 等位基因的 Cre 介导重组。我们通过将 Pomc-Cre 小鼠与 ROSA 报告品系杂交来可视化受这种转基因影响的群体,并在成年大脑中鉴定出 62 个重组部位,包括几个与能量平衡调节有关的核。为了比较急性 Pomc 启动子活性和 Pomc-Cre 介导的重组在单细胞水平上的关系,我们将 Pomc-增强型绿色荧光蛋白(eGFP)和 Pomc-Cre;ROSA-tdTomato 系进行了杂交。我们在下丘脑弓状核和齿状回中检测到最高浓度的 Pomc-eGFP+细胞,但也在孤束核、第三脑室室旁区和小脑观察到标记细胞的较小群体。与胚胎中 Pomc 表达的动态性质一致,在成年期,绝大多数用 tdTomato 报告基因标记的神经元在体内不表达 eGFP。因此,在使用 Pomc-Cre 转基因时,靶外部位的重组可能会导致生理表型。例如,我们发现,下丘脑弓状核中约 83%的对瘦素诱导的磷酸化信号转导和转录激活因子 3 有反应的细胞被 Pomc-Cre;ROSA-tdTomato 标记;只有 13%的这些是 eGFP+ POMC 神经元。

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