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不同生长锥群体中的可变膜糖蛋白。

Variable membrane glycoproteins in different growth cone populations.

作者信息

Li H N, Quiroga S, Pfenninger K H

机构信息

Department of Cellular and Structural Biology, University of Colorado School of Medicine, Denver.

出版信息

J Neurosci. 1992 Jun;12(6):2393-402. doi: 10.1523/JNEUROSCI.12-06-02393.1992.

Abstract

The question of whether growth cones generated by different neurons contain distinctive membrane glycoproteins was examined. Growth cone particles (GCPs) were isolated from specific regions of fetal or early postnatal brain, and their membrane proteins were analyzed by 2D gel electrophoresis and Western blotting, using WGA as a probe. These blots were compared to those generated by synaptosomes from adult brain. The patterns reveal a number of WGA-binding glycoproteins that are uniformly present in these subcellular fractions and others that are found in GCPs from selected brain regions only. The results indicate, therefore, substantial pattern diversity for the different, restricted growth cone populations. Some of the WGA-binding glycoproteins seen in GCPs disappear with increasing age and are absent from synaptosomes, while others seem to become more prominent. One of the glycoprotein complexes present in all GCP and synaptosome fractions analyzed is gp93. It has an apparent molecular weight of 90-97 kDa and exhibits unusually high heterogeneity in GCPs from whole fetal brain. The gp93 complex covers a pI range from about 4.9 to about 6.4 and consists of at least 12 different species, probably isoelectric variants. In GCPs from different brain regions, the sets of gp93 species observed are different and characteristic. Neuraminidase digestion shifts the gp93 pattern to a more neutral pI but simplifies it only partially, indicating that variable sialic acid content explains the molecular diversity to some extent. Thus, gp93 is a glycoprotein complex whose members are expressed and/or posttranslationally processed differentially in different growth cone populations. Such a glycoprotein family may be involved in selective cell-cell recognition.

摘要

研究了不同神经元产生的生长锥是否含有独特的膜糖蛋白这一问题。从胎儿或出生后早期大脑的特定区域分离出生长锥颗粒(GCPs),并使用WGA作为探针,通过二维凝胶电泳和蛋白质印迹法分析其膜蛋白。将这些印迹与成年大脑突触体产生的印迹进行比较。这些模式揭示了许多在这些亚细胞组分中均一存在的WGA结合糖蛋白,以及仅在选定脑区的GCPs中发现的其他糖蛋白。因此,结果表明不同的、受限的生长锥群体具有显著的模式多样性。在GCPs中观察到的一些WGA结合糖蛋白随着年龄增长而消失,并且在突触体中不存在,而其他一些糖蛋白似乎变得更加突出。在所有分析的GCP和突触体组分中存在的一种糖蛋白复合物是gp93。它的表观分子量为90 - 97 kDa,在整个胎儿大脑的GCPs中表现出异常高的异质性。gp93复合物的pI范围约为4.9至约6.4,由至少12种不同的物种组成,可能是等电变体。在来自不同脑区的GCPs中,观察到的gp93物种集是不同的且具有特征性。神经氨酸酶消化使gp93模式向更中性的pI移动,但仅部分简化,这表明可变的唾液酸含量在一定程度上解释了分子多样性。因此,gp93是一种糖蛋白复合物,其成员在不同的生长锥群体中差异表达和/或进行翻译后加工。这样的糖蛋白家族可能参与选择性细胞间识别。

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