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Cell-autonomous role of GFRα1 in the development of olfactory bulb GABAergic interneurons

机译:GFRα1在嗅球GABA能中间神经元发育中的细胞自主作用

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GFRα1, a receptor for glial cell line-derived neurotrophic factor (GDNF), is critical for the development of the main olfactory system. The olfactory bulb (OB) of Gfra1 knockout mice shows significant reductions in the number of olfactory sensory neurons, mitral and tufted cells, as well as all major classes of OB GABAergic interneurons. However, the latter do not express significant levels of GFRα1, leaving the mechanism of action of GFRα1 in OB interneuron development unexplained. Here we report that GFRα1 is highly expressed in the precursor cells that give rise to all major classes of OB interneurons, but is downregulated as these neurons mature. Conditional ablation of GFRα1 in embryonic GABAergic cells recapitulated the cell losses observed in global Gfra1 knockouts at birth. GFRα1 was also required for the sustained generation and allocation of OB interneurons in adulthood. Conditional loss of GFRα1 altered the migratory behaviour of neuroblasts along the rostral migratory stream (RMS) as well as RMS glial tunnel formation. Together, these data indicate that GFRα1 functions cell-autonomously in subpopulations of OB interneuron precursors to regulate their generation and allocation in the mammalian OB.
机译:GFRα1是神经胶质细胞系神经营养因子(GDNF)的受体,对于主要嗅觉系统的发育至关重要。 Gfra1基因敲除小鼠的嗅球(OB)显示嗅觉感觉神经元,二尖瓣和簇状细胞,以及所有主要类型的OB GABA能中神经元的数量显着减少。然而,后者并不表达显着水平的GFRα1,尚不清楚GFRα1在OB中间神经元发育中的作用机理。在这里我们报告说,GFRα1在前体细胞中高度表达,从而产生了所有主要类别的OB中间神经元,但随着这些神经元的成熟而被下调。胚胎GABA能细胞中GFRα1的条件消融概括了出生时整体Gfra1基因敲除中观察到的细胞损失。成年后OB中间神经元的持续生成和分配也需要GFRα1。 GFRα1的条件性损失改变了神经母细胞沿延髓迁徙流(RMS)以及RMS神经胶质隧道形成的迁徙行为。总之,这些数据表明,GFRα1在OB间神经元前体的亚群中具有细胞自主功能,以调节其在哺乳动物OB中的生成和分配。

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