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本文引用的文献

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Embryonic signaling centers expressing BMP, WNT and FGF proteins interact to pattern the cerebral cortex.表达骨形态发生蛋白(BMP)、Wnt 蛋白和纤维母细胞生长因子(FGF)的胚胎信号中心相互作用,从而确定大脑皮层的模式。
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EMX2 regulates sizes and positioning of the primary sensory and motor areas in neocortex by direct specification of cortical progenitors.EMX2通过直接指定皮质祖细胞来调节新皮质中主要感觉和运动区域的大小和位置。
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Loss of glutamatergic pyramidal neurons in frontal and temporal cortex resulting from attenuation of FGFR1 signaling is associated with spontaneous hyperactivity in mice.由于FGFR1信号减弱导致额叶和颞叶皮质中谷氨酸能锥体神经元的丧失与小鼠的自发活动亢进有关。
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FatiGO: a web tool for finding significant associations of Gene Ontology terms with groups of genes.FatiGO:一个用于查找基因本体术语与基因组之间显著关联的网络工具。
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An analysis of the gene expression program of mammalian neural progenitor cells.哺乳动物神经祖细胞基因表达程序的分析
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Generating the cerebral cortical area map.生成大脑皮质区域图谱。
Annu Rev Neurosci. 2003;26:355-80. doi: 10.1146/annurev.neuro.26.041002.131137.
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The murine Ten-m/Odz genes show distinct but overlapping expression patterns during development and in adult brain.
Gene Expr Patterns. 2003 Aug;3(4):397-405. doi: 10.1016/s1567-133x(03)00087-5.
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Emx2 patterns the neocortex by regulating FGF positional signaling.Emx2通过调节成纤维细胞生长因子(FGF)位置信号来塑造新皮质。
Nat Neurosci. 2003 Aug;6(8):825-31. doi: 10.1038/nn1093.
9
BMP ligands act redundantly to pattern the dorsal telencephalic midline.骨形态发生蛋白(BMP)配体在构建背侧端脑中线模式时发挥冗余作用。
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Early (E12) cortical progenitors can change their fate upon heterotopic transplantation.早期(胚胎第12天)的皮质祖细胞在异位移植后可改变其命运。
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基于Fgf调节梯度的新皮质原图谱的基因组特征分析。

Genomic characterisation of a Fgf-regulated gradient-based neocortical protomap.

作者信息

Sansom Stephen N, Hébert Jean M, Thammongkol Uruporn, Smith James, Nisbet Grace, Surani M Azim, McConnell Susan K, Livesey Frederick J

机构信息

Wellcome Trust/CR UK Gurdon Institute, University of Cambridge, Tennis Court Road, Cambridge CB2 1QN, UK.

出版信息

Development. 2005 Sep;132(17):3947-61. doi: 10.1242/dev.01968. Epub 2005 Aug 3.

DOI:10.1242/dev.01968
PMID:16079153
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4729368/
Abstract

Recent findings support a model for neocortical area formation in which neocortical progenitor cells become patterned by extracellular signals to generate a protomap of progenitor cell areas that in turn generate area-specific neurons. The protomap is thought to be underpinned by spatial differences in progenitor cell identity that are reflected at the transcriptional level. We systematically investigated the nature and composition of the protomap by genomic analyses of spatial and temporal neocortical progenitor cell gene expression. We did not find gene expression evidence for progenitor cell organisation into domains or compartments, instead finding rostrocaudal gradients of gene expression across the entire neocortex. Given the role of Fgf signalling in rostrocaudal neocortical patterning, we carried out an in vivo global analysis of cortical gene expression in Fgfr1 mutant mice, identifying consistent alterations in the expression of candidate protomap elements. One such gene, Mest, was predicted by those studies to be a direct target of Fgf8 signalling and to be involved in setting up, rather than implementing, the progenitor cell protomap. In support of this, we confirmed Mest as a direct transcriptional target of Fgf8-regulated signalling in vitro. Functional studies demonstrated that this gene has a role in establishing patterned gene expression in the developing neocortex, potentially by acting as a negative regulator of the Fgf8-controlled patterning system.

摘要

最近的研究结果支持一种新皮质区域形成模型,在该模型中,新皮质祖细胞通过细胞外信号形成模式,以生成祖细胞区域的原图谱,进而产生区域特异性神经元。原图谱被认为是由祖细胞身份的空间差异所支撑,这种差异在转录水平上得以体现。我们通过对新皮质祖细胞基因表达的时空基因组分析,系统地研究了原图谱的性质和组成。我们没有发现基因表达证据表明祖细胞组织成区域或隔室,而是发现整个新皮质中基因表达存在前后梯度。鉴于Fgf信号在新皮质前后模式形成中的作用,我们对Fgfr1突变小鼠的皮质基因表达进行了体内全局分析,确定了候选原图谱元件表达的一致变化。这些研究预测,其中一个这样的基因Mest是Fgf8信号的直接靶点,并且参与建立而非实施祖细胞原图谱。为此,我们在体外证实Mest是Fgf8调节信号的直接转录靶点。功能研究表明,该基因可能通过作为Fgf8控制的模式系统的负调节因子,在发育中的新皮质中建立模式化基因表达方面发挥作用。