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首页> 外文期刊>The biochemical journal >Carbohydrate structures of the human-immunodeficiency-virus (HIV) recombinant envelope glycoprotein gp120 produced in Chinese-hamster ovary cells
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Carbohydrate structures of the human-immunodeficiency-virus (HIV) recombinant envelope glycoprotein gp120 produced in Chinese-hamster ovary cells

机译:中国仓鼠卵巢细胞中产生的人免疫缺陷病毒(HIV)重组包膜糖蛋白gp120的碳水化合物结构

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pThe present paper describes the structures of the N-linked oligosaccharides of the human-immunodeficiency-virus (HIV) envelope glycoprotein gp120 (cloned from the HTLV-III B isolate and expressed as a secreted fusion protein after transfection of Chinese-hamster ovary cells), which is known to bind with high affinity to human T4-lymphocytes. Oligosaccharides were released from peptide by hydrazinolysis, fractionated by paper electrophoresis, high-performance lectin-affinity chromatography and Bio-Gel P-4 column chromatography, and their structures determined by sequential exoglycosidase digestions in conjunction with methylation analysis. The glycoprotein was found to be unique in its diversity of oligosaccharide structures. These include high-mannose type and hybrid type, as well as four categories of complex-type chains: mono-, bi-, tri- and tetra-antennary, with or without N-acetyl-lactosamine repeats, and with or without a core-region fucose residue. Among the sialidase-treated oligosaccharides, no less than 29 structures were identified as follows: (formula; see text) where G is galactose, GN is N-acetylglucosamine, M is mannose, F is fucose, and ‘+/- ’ means that residues are present in a proportion of chains. The actual number of oligosaccharide structures is much greater, since before desialylation there was evidence that, among the hybrid and complex-type chains, all but 6% contained sialic acid at the C-3 position of terminal galactose residues, and partially sialylated forms of the bi- and multi-antennary chains were present. Detailed evidence for the proposed oligosaccharide sequences will be published as a supplementary paper [T. Mizuochi, M. W. Spellman, M. Larkin, J. Solomon, L. J. Basa & T. Feizi (1988) Biomed. Chromatogr., in the press]./p
机译:>本文描述了人免疫缺陷病毒(HIV)包膜糖蛋白gp120(从HTLV-III B分离株克隆并在转染中国仓鼠后表达为分泌的融合蛋白)的N-连接寡糖的结构卵巢细胞),已知与人T4淋巴细胞具有高亲和力。寡糖通过肼解作用从肽中释放出来,通过纸电泳,高效凝集素亲和色谱和Bio-Gel P-4柱色谱进行分离,并通过连续的糖苷外切酶消化和甲基化分析确定其结构。发现该糖蛋白在寡糖结构的多样性方面是独特的。这些包括高甘露糖型和杂合型,以及四类复杂类型的链:单,双,三和四触角,带有或不带有N-乙酰-乳糖胺重复序列,带有或不带有核心区岩藻糖残基。在经唾液酸酶处理的寡糖中,鉴定出不少于29个结构,如下所示:(分子式;见正文)其中G为半乳糖,GN为N-乙酰氨基葡萄糖,M为甘露糖,F为岩藻糖,“ +/-”表示残基以一定比例的链存在。寡糖结构的实际数目要多得多,因为在去唾液酸化之前,有证据表明,在杂合型和复杂型链中,除6%以外,所有都在末端半乳糖残基的C-3位上含有唾液酸,以及部分唾液酸化形式。存在双天线链和多天线链。拟议的寡糖序列的详细证据将作为补充论文[T. Mizuochi,M。W. Spellman,M。Larkin,J。Solomon,L。J. Basa& T.Feizi(1988)生物医学。色谱,请按]。

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