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血管内皮生长因子同工型的变化导致与早期神经干细胞增殖和分化相关的转录组变化在小鼠前脑中。

Shifts in the vascular endothelial growth factor isoforms result in transcriptome changes correlated with early neural stem cell proliferation and differentiation in mouse forebrain.

机构信息

Department of Biology, University of North Dakota, Grand Forks, North Dakota.

出版信息

Dev Neurobiol. 2014 Jan;74(1):63-81. doi: 10.1002/dneu.22130. Epub 2013 Nov 4.

DOI:10.1002/dneu.22130
PMID:24124161
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4096862/
Abstract

Regulation of neural stem cell (NSC) fate decisions is critical during the transition from a multicellular mammalian forebrain neuroepithelium to the multilayered neocortex. Forebrain development requires coordinated vascular investment alongside NSC differentiation. Vascular endothelial growth factor A (Vegf) has proven to be a pleiotrophic gene whose multiple protein isoforms regulate a broad range of effects in neurovascular systems. To test the hypothesis that the Vegf isoforms (120, 164, and 188) are required for normal forebrain development, we analyzed the forebrain transcriptome of mice expressing specific Vegf isoforms, Vegf120, VegfF188, or a combination of Vegf120/188. Transcriptome analysis identified differentially expressed genes in embryonic day (E) 9.5 forebrain, a time point preceding dramatic neuroepithelial expansion and vascular investment in the telencephalon. Meta-analysis identified gene pathways linked to chromosome-level modifications, cell fate regulation, and neurogenesis that were altered in Vegf isoform mice. Based on these gene network shifts, we predicted that NSC populations would be affected in later stages of forebrain development. In the E11.5 telencephalon, we quantified mitotic cells [Phospho-Histone H3 (pHH3)-positive] and intermediate progenitor cells (Tbr2/Eomes-positive), observing quantitative and qualitative shifts in these populations. We observed qualitative shifts in cortical layering at P0, particularly with Ctip2-positive cells in layer V. The results identify a suite of genes and functional gene networks that can be used to further dissect the role of Vegf in regulating NSC differentiation and downstream consequences for NSC fate decisions.

摘要

神经干细胞(NSC)命运决定的调节在从多细胞哺乳动物前脑神经上皮到多层新皮层的转变过程中至关重要。前脑发育需要与 NSC 分化相协调的血管投资。血管内皮生长因子 A(Vegf)已被证明是一种多功能基因,其多种蛋白同工型调节神经血管系统的广泛作用。为了检验 Vegf 同工型(120、164 和 188)对于正常前脑发育是必需的假说,我们分析了表达特定 Vegf 同工型(Vegf120、VegfF188 或 Vegf120/188 的组合)的小鼠的前脑转录组。转录组分析确定了胚胎日(E)9.5 前脑的差异表达基因,这是一个在端脑神经上皮剧烈扩张和血管投资之前的时间点。荟萃分析确定了与染色体水平修饰、细胞命运调节和神经发生相关的基因途径,这些途径在 Vegf 同工型小鼠中发生了改变。基于这些基因网络的转变,我们预测 NSC 群体在前脑发育的后期阶段会受到影响。在 E11.5 端脑中,我们定量了有丝分裂细胞[磷酸组蛋白 H3(pHH3)阳性]和中间祖细胞(Tbr2/Eomes 阳性),观察到这些群体的数量和质量发生了变化。在 P0 时,我们观察到皮质分层的定性变化,特别是在 V 层中 Ctip2 阳性细胞。这些结果确定了一套基因和功能基因网络,可以进一步剖析 Vegf 在调节 NSC 分化和 NSC 命运决定的下游后果中的作用。

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