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胚胎小鼠前脑中表达neogenin的神经祖细胞群体和迁移神经母细胞的特征分析。

Characterization of neogenin-expressing neural progenitor populations and migrating neuroblasts in the embryonic mouse forebrain.

作者信息

Fitzgerald D P, Cole S J, Hammond A, Seaman C, Cooper H M

机构信息

Queensland Brain Institute, Neural Migration Laboratory, The University of Queensland, St. Lucia, Brisbane, Queensland 4072, Australia.

出版信息

Neuroscience. 2006 Oct 27;142(3):703-16. doi: 10.1016/j.neuroscience.2006.06.041. Epub 2006 Aug 14.

Abstract

Many studies have demonstrated a role for netrin-1-deleted in colorectal cancer (DCC) interactions in both axon guidance and neuronal migration. Neogenin, a member of the DCC receptor family, has recently been shown to be a chemorepulsive axon guidance receptor for the repulsive guidance molecule (RGM) family of guidance cues [Rajagopalan S, Deitinghoff L, Davis D, Conrad S, Skutella T, Chedotal A, Mueller B, Strittmatter S (2004) Neogenin mediates the action of repulsive guidance molecule. Nat Cell Biol 6:755-762]. Here we show that neogenin is present on neural progenitors, including neurogenic radial glia, in the embryonic mouse forebrain suggesting that neogenin expression is a hallmark of neural progenitor populations. Neogenin-positive progenitors were isolated from embryonic day 14.5 forebrain using flow cytometry and cultured as neurospheres. Neogenin-positive progenitors gave rise to neurospheres displaying a high proliferative and neurogenic potential. In contrast, neogenin-negative forebrain cells did not produce long-term neurosphere cultures and did not possess a significant neurogenic potential. These observations argue strongly for a role for neogenin in neural progenitor biology. In addition, we also observed neogenin on parvalbumin- and calbindin-positive interneuron neuroblasts that were migrating through the medial and lateral ganglionic eminences, suggesting a role for neogenin in tangential migration. Therefore, neogenin may be a multi-functional receptor regulating both progenitor activity and neuroblast migration in the embryonic forebrain.

摘要

许多研究已证明,在轴突导向和神经元迁移过程中,结直肠癌缺失的netrin-1(DCC)相互作用发挥了作用。DCC受体家族成员新生蛋白(Neogenin)最近被证明是排斥性导向分子(RGM)家族导向线索的一种化学排斥性轴突导向受体[拉贾戈帕兰S,戴廷霍夫L,戴维斯D,康拉德S,斯库特拉T,谢多塔尔A,米勒B,斯特里特马特S(2004年)新生蛋白介导排斥性导向分子的作用。《自然细胞生物学》6:第755 - 762页]。在此我们表明,新生蛋白存在于胚胎小鼠前脑的神经祖细胞上,包括神经源性放射状胶质细胞,这表明新生蛋白的表达是神经祖细胞群体的一个标志。使用流式细胞术从胚胎第14.5天的前脑中分离出新生蛋白阳性祖细胞,并培养成神经球。新生蛋白阳性祖细胞产生了具有高增殖和神经源性潜能的神经球。相比之下,新生蛋白阴性的前脑细胞不能产生长期的神经球培养物,也不具有显著的神经源性潜能。这些观察结果有力地证明了新生蛋白在神经祖细胞生物学中的作用。此外,我们还在通过内侧和外侧神经节隆起迁移的小白蛋白和钙结合蛋白阳性中间神经元神经母细胞上观察到了新生蛋白,这表明新生蛋白在切向迁移中发挥作用。因此,新生蛋白可能是一种多功能受体,调节胚胎前脑中的祖细胞活性和神经母细胞迁移。

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