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糖基磷脂酰肌醇(GPI)锚定蛋白在细胞表面的积累需要在多个细胞内水平进行分选。

Accumulation of a GPI-anchored protein at the cell surface requires sorting at multiple intracellular levels.

作者信息

Grünfelder Christoph G, Engstler Markus, Weise Frank, Schwarz Heinz, Stierhof York-Dieter, Boshart Michael, Overath Peter

机构信息

Max-Planck-Institut für Biologie, Abteilung Membranbiochemie, Corrensstrasse 38, D-72076 Tübingen, Germany.

出版信息

Traffic. 2002 Aug;3(8):547-59. doi: 10.1034/j.1600-0854.2002.30805.x.

Abstract

Proteins modified by glycosylphosphatidylinositol membrane anchors have become popular for investigating the role of membrane lipid microdomains in cellular sorting processes. To this end, trypanosomatids offer the advantage that they express these molecules in high abundance. The parasitic protozoan Trypanosoma brucei is covered by a dense and nearly homogeneous coat composed of a glycosylphosphatidylinositol-anchored protein, the variant surface glycoprotein, which is essential for survival of the parasite in the mammalian blood. Therefore, T. brucei must possess mechanisms to selectively and efficiently deliver variant surface glycoprotein to the cell surface. In this study, we have quantified the steady-state distribution of variant surface glycoprotein by differential biotinylation, by fluorescence microscopy and by immunoelectron microscopy on high-pressure frozen and freeze-substituted samples. These three techniques provide very similar estimates of the fraction of variant surface glycoprotein located on the cell surface, on average 89.4%. The intracellular variant surface glycoprotein (10.6%) is predominantly located in the endosomal compartment (75%), while 25% are associated with the endoplasmic reticulum, Golgi apparatus and lysosomes. The density of variant surface glycoprotein in the plasma membrane including the membrane of the flagellar pocket, the only site for endo- and exocytosis in this organism, is 48-52 times higher than the density in endoplasmic reticulum membranes. The relative densities of the Golgi complex and of the endosomes are 2.7 and 10.8, respectively, compared to the endoplasmic reticulum. This data set provides the basis for an analysis of the dynamics of sorting. Depending on the intracellular itinerary of newly formed variant surface glycoprotein, the high surface density is achieved in two (endoplasmic reticulum --> Golgi complex --> cell surface) or three enrichment steps (endoplasmic reticulum --> Golgi complex --> endosomes --> cell surface), suggesting sorting between several membrane compartments.

摘要

糖基磷脂酰肌醇膜锚修饰的蛋白质已成为研究膜脂微区在细胞分选过程中作用的热门对象。为此,锥虫具有表达这些分子数量丰富的优势。寄生原生动物布氏锥虫表面覆盖着一层致密且几乎均匀的被膜,该被膜由糖基磷脂酰肌醇锚定蛋白——可变表面糖蛋白组成,这对寄生虫在哺乳动物血液中的存活至关重要。因此,布氏锥虫必须具备将可变表面糖蛋白选择性且高效地转运至细胞表面的机制。在本研究中,我们通过差异生物素化、荧光显微镜以及对高压冷冻和冷冻替代样品进行免疫电子显微镜观察,对可变表面糖蛋白的稳态分布进行了定量分析。这三种技术对位于细胞表面的可变表面糖蛋白比例提供了非常相似的估计值,平均为89.4%。细胞内的可变表面糖蛋白(10.6%)主要位于内体区室(75%),而25%与内质网、高尔基体和溶酶体相关。包括鞭毛袋膜(该生物体中唯一的内吞和外排位点)在内的质膜中可变表面糖蛋白的密度比内质网膜中的密度高48 - 52倍。与内质网相比,高尔基体复合体和内体的相对密度分别为2.7和10.8。该数据集为分析分选动力学提供了基础。根据新形成可变表面糖蛋白的细胞内行程,高表面密度可通过两个(内质网→高尔基体复合体→细胞表面)或三个富集步骤(内质网→高尔基体复合体→内体→细胞表面)实现,这表明在几个膜区室之间存在分选过程。

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