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缺乏神经节苷脂生物合成基因B4galnt1的小鼠运动皮层和齿状颗粒细胞的树突形态和棘密度未改变——一项定量高尔基染色法研究

Dendritic morphology and spine density is not altered in motor cortex and dentate granular cells in mice lacking the ganglioside biosynthetic gene B4galnt1 - A quantitative Golgi cox study.

作者信息

Dobrović Branko, Curić Goran, Petanjek Zdravko, Heffer Marija

机构信息

University of Zagreb, Croatian Institute for Brain Research, Zagreb, Croatia.

出版信息

Coll Antropol. 2011 Jan;35 Suppl 1:25-30.

PMID:21648307
Abstract

Gangliosides are characteristic plasma membrane constituents of vertebrate brain used as milestones of neuronal development. As neuronal morphology is a good indicator of neuronal differentiation, we analyzed how lack of the ganglioside biosynthetic gene Galgt1 whose product is critical for production of four major adult mammalian brain complex gangliosides (GM1, GD1a, GD1b and GT1b) affects neuronal maturation in vivo. To define maturation of cortical neurons in mice lacking B4galnt1 we performed a morphological analysis of Golgi-Cox impregnated pyramidal neurons in primary motor cortex and granular cells of dentate gyrus in 3, 21 and 150 days old B4galnt1-null and wild type mice. Quantitative analysis of basal dendritic tree on layer III pyramidal neurons in the motor cortex showed very immature dendritic picture in both mice at postnatal day 3. At postnatal day 21 both mice reached adult values in dendritic length, complexity and spine density. No quantitative differences were found between B4galnt1-null and wild type mice in pyramidal cells of motor cortex or granular cells of dentate gyrus at any examined age. In addition, the general structural and neuronal organization of all brain structures, qualitatively observed on Nissl and Golgi-Cox, were similar Our results demonstrate that neurons can develop normal dendritic complexity and length without presence of complex gangliosides in vivo. Therefore, behavioral differences observed in B4galnt1-null mice may be attributed to functional rather than morphological level of dendrites and spines of cortical pyramidal neurons.

摘要

神经节苷脂是脊椎动物大脑特有的质膜成分,用作神经元发育的标志物。由于神经元形态是神经元分化的良好指标,我们分析了神经节苷脂生物合成基因Galgt1的缺失如何影响体内神经元的成熟,该基因的产物对四种主要的成年哺乳动物脑复合神经节苷脂(GM1、GD1a、GD1b和GT1b)的产生至关重要。为了确定缺乏B4galnt1的小鼠中皮质神经元的成熟情况,我们对3日龄、21日龄和150日龄的B4galnt1基因敲除小鼠和野生型小鼠的初级运动皮质中高尔基-考克斯染色的锥体神经元以及齿状回颗粒细胞进行了形态学分析。对运动皮质III层锥体神经元基底树突的定量分析显示,出生后第3天,两种小鼠的树突形态都非常不成熟。出生后第21天,两种小鼠的树突长度、复杂性和棘密度均达到成年水平。在任何检查年龄,B4galnt1基因敲除小鼠和野生型小鼠在运动皮质的锥体细胞或齿状回颗粒细胞中均未发现定量差异。此外,在尼氏染色和高尔基-考克斯染色中定性观察到的所有脑结构的总体结构和神经元组织相似。我们的结果表明,在体内没有复合神经节苷脂的情况下,神经元也可以发育出正常的树突复杂性和长度。因此,在B4galnt1基因敲除小鼠中观察到的行为差异可能归因于皮质锥体神经元树突和棘的功能水平而非形态水平。

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