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早期新皮层发育过程中 Eomes+ 谱系兴奋性神经元中基因表达模式的层次聚类。

Hierarchical clustering of gene expression patterns in the Eomes + lineage of excitatory neurons during early neocortical development.

机构信息

Department of Neuroscience and Physiology, SUNY Upstate Medical University, Syracuse, NY 13210, USA.

出版信息

BMC Neurosci. 2012 Aug 1;13:90. doi: 10.1186/1471-2202-13-90.

Abstract

BACKGROUND

Cortical neurons display dynamic patterns of gene expression during the coincident processes of differentiation and migration through the developing cerebrum. To identify genes selectively expressed by the Eomes + (Tbr2) lineage of excitatory cortical neurons, GFP-expressing cells from Tg(Eomes::eGFP) Gsat embryos were isolated to > 99% purity and profiled.

RESULTS

We report the identification, validation and spatial grouping of genes selectively expressed within the Eomes + cortical excitatory neuron lineage during early cortical development. In these neurons 475 genes were expressed ≥ 3-fold, and 534 genes ≤ 3-fold, compared to the reference population of neuronal precursors. Of the up-regulated genes, 328 were represented at the Genepaint in situ hybridization database and 317 (97%) were validated as having spatial expression patterns consistent with the lineage of differentiating excitatory neurons. A novel approach for quantifying in situ hybridization patterns (QISP) across the cerebral wall was developed that allowed the hierarchical clustering of genes into putative co-regulated groups. Forty four candidate genes were identified that show spatial expression with Intermediate Precursor Cells, 49 candidate genes show spatial expression with Multipolar Neurons, while the remaining 224 genes achieved peak expression in the developing cortical plate.

CONCLUSIONS

This analysis of differentiating excitatory neurons revealed the expression patterns of 37 transcription factors, many chemotropic signaling molecules (including the Semaphorin, Netrin and Slit signaling pathways), and unexpected evidence for non-canonical neurotransmitter signaling and changes in mechanisms of glucose metabolism. Over half of the 317 identified genes are associated with neuronal disease making these findings a valuable resource for studies of neurological development and disease.

摘要

背景

皮质神经元在通过发育中的大脑进行分化和迁移的同时,表现出动态的基因表达模式。为了鉴定 Eomes + (Tbr2)兴奋性皮质神经元谱系特异性表达的基因,从 Tg(Eomes::eGFP) Gsat 胚胎的 GFP 表达细胞中分离出 > 99%纯度的细胞进行分析。

结果

我们报告了在早期皮质发育过程中,Eomes + 皮质兴奋性神经元谱系中选择性表达的基因的鉴定、验证和空间分组。在这些神经元中,与神经元前体的参考群体相比,有 475 个基因的表达≥ 3 倍,有 534 个基因的表达≤ 3 倍。上调基因中,328 个在 Genepaint 原位杂交数据库中有代表,317 个(97%)被验证为具有与分化兴奋性神经元谱系一致的空间表达模式。开发了一种新的定量原位杂交模式(QISP)方法,可在大脑壁上对基因进行层次聚类,将基因分为可能的共调控组。鉴定出 44 个候选基因具有与中间前体细胞的空间表达,49 个候选基因具有与多极神经元的空间表达,而其余 224 个基因在发育中的皮质板中表达达到峰值。

结论

这项对分化兴奋性神经元的分析揭示了 37 个转录因子、许多趋化信号分子(包括 Semaphorin、Netrin 和 Slit 信号通路)的表达模式,以及非经典神经递质信号和葡萄糖代谢机制变化的意外证据。鉴定出的 317 个基因中有一半以上与神经疾病有关,这使得这些发现成为神经发育和疾病研究的宝贵资源。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f8ca/3583225/bad89a0e4ef8/1471-2202-13-90-1.jpg

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