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中间祖细胞和 Tbr2 在皮质发育中的作用。

Intermediate progenitors and Tbr2 in cortical development.

机构信息

Department of Pathology, University of California, San Diego, CA, USA.

出版信息

J Anat. 2019 Sep;235(3):616-625. doi: 10.1111/joa.12939. Epub 2019 Jan 24.

DOI:10.1111/joa.12939
PMID:30677129
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6656625/
Abstract

In developing cerebral cortex, intermediate progenitors (IPs) are transit amplifying cells that specifically express Tbr2 (gene: Eomes), a T-box transcription factor. IPs are derived from radial glia (RG) progenitors, the neural stem cells of developing cortex. In turn, IPs generate glutamatergic projection neurons (PNs) exclusively. IPs are found in ventricular and subventricular zones, where they differentiate as distinct ventricular IP (vIP) and outer IP (oIP) subtypes. Morphologically, IPs have short processes, resembling filopodia or neurites, that transiently contact other cells, most importantly dividing RG cells to mediate Delta-Notch signaling. Also, IPs secrete a chemokine, Cxcl12, which guides interneuron and microglia migrations and promotes thalamocortical axon growth. In mice, IPs produce clones of 1-12 PNs, sometimes spanning multiple layers. After mitosis, IP daughter cells undergo asymmetric cell death in the majority of instances. In mice, Tbr2 is necessary for PN differentiation and subtype specification, and to repress IP-genic transcription factors. Tbr2 directly represses Insm1, an IP-genic transcription factor gene, as well as Pax6, a key activator of Tbr2 transcription. Without Tbr2, abnormal IPs transiently accumulate in elevated numbers. More broadly, Tbr2 regulates the transcriptome by activating or repressing hundreds of direct target genes. Notably, Tbr2 'unlocks' and activates PN-specific genes, such as Tbr1, by recruiting Jmjd3, a histone H3K27me3 demethylase that removes repressive epigenetic marks placed by polycomb repressive complex 2. IPs have played an important role in the evolution and gyrification of mammalian cerebral cortex, and TBR2 is essential for human brain development.

摘要

在大脑皮层发育过程中,中间祖细胞(IPs)是一种过渡扩增细胞,其特异性表达 Tbr2(基因:Eomes),一种 T 盒转录因子。IPs 起源于放射状胶质(RG)祖细胞,是皮质发育中的神经干细胞。反过来,IPs 专门产生谷氨酸能投射神经元(PNs)。IPs 存在于脑室和脑室下区,在那里它们分化为不同的脑室 IP(vIP)和外 IP(oIP)亚型。形态上,IPs 具有短的突起,类似于丝状伪足或神经突,它们暂时与其他细胞接触,最重要的是与正在分裂的 RG 细胞接触,以介导 Delta-Notch 信号。此外,IPs 分泌趋化因子 Cxcl12,该因子指导中间神经元和小胶质细胞迁移,并促进丘脑皮质轴突生长。在小鼠中,IPs 产生 1-12 个 PNs 的克隆,有时跨越多个皮层层。有丝分裂后,大多数情况下 IP 子细胞经历不对称细胞死亡。在小鼠中,Tbr2 对于 PN 分化和亚型特化以及抑制 IP 发生转录因子是必需的。Tbr2 直接抑制 IP 发生转录因子基因 Insm1 和 Pax6,后者是 Tbr2 转录的关键激活子。没有 Tbr2,异常的 IPs 会短暂地大量积累。更广泛地说,Tbr2 通过激活或抑制数百个直接靶基因来调节转录组。值得注意的是,Tbr2 通过招募组蛋白 H3K27me3 去甲基酶 Jmjd3,“解锁”并激活 PN 特异性基因,如 Tbr1,去除多梳抑制复合物 2 放置的抑制性表观遗传标记。IPs 在哺乳动物大脑皮层的进化和脑回形成中发挥了重要作用,而 TBR2 对于人类大脑发育是必不可少的。

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