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密切相关的鼠白血病病毒糖基化模式的差异。

Differences in glycosylation patterns of closely related murine leukemia viruses.

作者信息

Rosner M R, Grinna L S, Robbins P W

出版信息

Proc Natl Acad Sci U S A. 1980 Jan;77(1):67-71. doi: 10.1073/pnas.77.1.67.

Abstract

The nature of the carbohydrate chains in the major envelope glycoprotein of murine leukemia virus, gp70, and its cellular precursor has been investigated. A difference in the oligosaccharide composition of gp70 from an ecotropic murine leukemia virus (Akv) and three recombinant dual-tropic viruses [mink cell focus-inducing viruses (MCFs)] derived from Akv was demonstrated. Glycosidase digestion and gel filtration were utilized to identify the two classes of N-asparagine-linked oligosaccharides, high-mannose and complex. The gp70 of the ecotropic virus contained only N-linked oligosaccharides of the complex type. In contrast, the gp70s of the dual-tropic viruses contained both high-mannose and complex oligosaccharides. Analysis of gp70 glycopeptides from an MCF-related xenotropic virus showed an elution profile similar, but not identical, to profiles of the MCFs. The gp70 precursors isolated from cells infected with Akv or MCF virus contained N-linked oligosaccharides that were exclusively of the high-mannose type. Comparison of the high-mannose oligosaccharides of the MCF gp70 precursors with those of the corresponding gp70s indicated that very little further processing of the high-mannose residues in the gp70s had occurred. The presence of the high-mannose oligosaccharides in the envelope glycoprotein of the dual-tropic viruses results from altered carbohydrate processing. The conservation of this altered carbohydrate pattern in a number of hosts and under various conditions of growth suggests that the viral protein structure is the primary factor in determining the different mode of glycosylation of the MCF gp70s. Thus, these viral glycoproteins provide an important model system for studying the relationship between protein structure and patterns of glycosylation.

摘要

对小鼠白血病病毒主要包膜糖蛋白gp70及其细胞前体中的碳水化合物链的性质进行了研究。已证明来自亲嗜性小鼠白血病病毒(Akv)的gp70与三种源自Akv的重组双嗜性病毒[貂细胞聚焦诱导病毒(MCF)]的寡糖组成存在差异。利用糖苷酶消化和凝胶过滤来鉴定两类与天冬酰胺连接的寡糖,即高甘露糖型和复合型。亲嗜性病毒的gp70仅含有复合型的N-连接寡糖。相比之下,双嗜性病毒的gp70既含有高甘露糖型寡糖,也含有复合型寡糖。对一种与MCF相关的异嗜性病毒的gp70糖肽分析显示,其洗脱图谱与MCF的洗脱图谱相似但不完全相同。从感染Akv或MCF病毒的细胞中分离出的gp70前体含有仅为高甘露糖型的N-连接寡糖。将MCF gp70前体的高甘露糖型寡糖与相应gp70的高甘露糖型寡糖进行比较表明,gp70中高甘露糖残基的进一步加工很少发生。双嗜性病毒包膜糖蛋白中高甘露糖型寡糖的存在是碳水化合物加工改变的结果。这种改变的碳水化合物模式在许多宿主中以及在各种生长条件下都得以保留,这表明病毒蛋白结构是决定MCF gp70不同糖基化模式的主要因素。因此,这些病毒糖蛋白为研究蛋白质结构与糖基化模式之间的关系提供了一个重要的模型系统。

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