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皮质中间神经元前体细胞中的基因表达预示着它们的成熟功能。

Gene expression in cortical interneuron precursors is prescient of their mature function.

作者信息

Batista-Brito Renata, Machold Robert, Klein Corinna, Fishell Gord

机构信息

Smilow Neuroscience Program and the Department of Cell Biology, Smilow Research Building, New York University Medical Center, 522 First Avenue, New York, NY 10016, USA.

出版信息

Cereb Cortex. 2008 Oct;18(10):2306-17. doi: 10.1093/cercor/bhm258. Epub 2008 Feb 3.

DOI:10.1093/cercor/bhm258
PMID:18250082
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2536702/
Abstract

At present little is known about the developmental mechanisms that give rise to inhibitory gamma-aminobutyric acidergic interneurons of the neocortex or the timing of their subtype specification. As such, we performed a gene expression microarray analysis on cortical interneuron precursors isolated through their expression of a Dlx5/6(Cre-IRES-EGFP) transgene. We purified these precursors from the embryonic mouse neocortex at E13.5 and E15.5 by sorting of enhanced green fluorescent protein-expressing cells. We identified novel transcription factors, neuropeptides, and cell surface genes whose expression is highly enriched in embryonic cortical interneuron precursors. Our identification of many of the genes known to be selectively enriched within cortical interneurons validated the efficacy of our approach. Surprisingly, we find that subpopulations of migrating cortical interneurons express genes encoding for proteins characteristic of mature interneuron subtypes as early as E13.5. These results provide support for the idea that many of the genes characteristic of specific cortical interneuron subtypes are evident prior to their functional integration into cortical microcircuitry. They suggest interneurons are already relegated to specific genetic subtypes shortly after they become postmitotic. Moreover, our work has revealed that many of the genes expressed in cortical interneuron precursors have been independently linked to neurological disorders in both mice and humans.

摘要

目前,对于产生新皮层抑制性γ-氨基丁酸能中间神经元的发育机制及其亚型特化的时间知之甚少。因此,我们对通过表达Dlx5/6(Cre-IRES-EGFP)转基因而分离出的皮层中间神经元前体细胞进行了基因表达微阵列分析。我们在胚胎第13.5天和第15.5天,通过对表达增强型绿色荧光蛋白的细胞进行分选,从胚胎小鼠新皮层中纯化出这些前体细胞。我们鉴定出了新的转录因子、神经肽和细胞表面基因,它们在胚胎皮层中间神经元前体细胞中的表达高度富集。我们对许多已知在皮层中间神经元中选择性富集的基因的鉴定,验证了我们方法的有效性。令人惊讶的是,我们发现早在胚胎第13.5天,迁移中的皮层中间神经元亚群就表达了编码成熟中间神经元亚型特征性蛋白质的基因。这些结果支持了这样一种观点,即特定皮层中间神经元亚型的许多特征性基因在其功能整合到皮层微回路之前就已显现。这表明中间神经元在成为有丝分裂后不久就已被归入特定的基因亚型。此外,我们的研究表明,在皮层中间神经元前体细胞中表达的许多基因,在小鼠和人类中都已被独立地与神经系统疾病联系起来。

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Gene copy number variation in schizophrenia.精神分裂症中的基因拷贝数变异
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