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中国仓鼠卵巢细胞Lec9突变体中Man5GlcNAc2-P-P-脂质的利用减少:寡糖-脂质组装步骤的分析。

Reduced utilization of Man5GlcNAc2-P-P-lipid in a Lec9 mutant of Chinese hamster ovary cells: analysis of the steps in oligosaccharide-lipid assembly.

作者信息

Hall C W, McLachlan K R, Krag S S, Robbins A R

机构信息

Laboratory of Biochemistry and Metabolism, NIDDK, National Institutes of Health, Bethesda, Maryland 20892, USA.

出版信息

J Cell Biochem. 1997 Nov 1;67(2):201-15.

PMID:9328825
Abstract

Recently we reported that CHB11-1-3, a Chinese hamster ovary cell mutant defective in glycosylation of asparagine-linked proteins, is defective in the synthesis of dolichol [Quellhorst et al., 343:19-26, 1997: Arch Biochem Biophys]. CHB11-1-3 was found to be in the Lec9 complementation group, which synthesizes polyprenol rather than dolichol. In this paper, levels of various polyprenyl derivatives in CHB11-1-3 are compared to levels of the corresponding dolichyl derivatives in parental cells. CHB11-1-3 was found to maintain near normal levels of Man5GlcNAc2-P-P-polyprenol and mannosylphosphorylpolyprenol, despite reduced rates of synthesis, by utilizing those intermediates at a reduced rate. The Man5GlcNAc2 oligosaccharide attached to prenol in CHB11-1-3 cells and to dolichol in parental cells is the same structure, as determined by acetolysis. Man5GlcNAc2-P-P-polyprenol and Man5GlcNAc5-P-P-dolichol both appeared to be translocated efficiently in an in vitro reaction. Glycosylation of G protein was compared in vesicular stomatitus virus (VSV)-infected parent and mutant; although a portion of G protein was compared in vesicular stomatitus virus (VSV)-infected parent and mutant; although a portion of G protein was normally glycosylated in CHB11-1-3 cells, a large portion of G was underglycosylated, resulting in the addition of either one or no oligosaccharide to G. Addition of a single oligosaccharide occurred randomly rather than preferentially at one of the two sites.

摘要

最近我们报道,中国仓鼠卵巢细胞突变体CHB11 - 1 - 3在天冬酰胺连接蛋白糖基化方面存在缺陷,其在多萜醇合成方面也存在缺陷[Quellhorst等人,《生物化学与生物物理学报》343:19 - 26,1997年]。发现CHB11 - 1 - 3属于Lec9互补组,该组合成聚戊烯醇而非多萜醇。在本文中,将CHB11 - 1 - 3中各种聚戊烯基衍生物的水平与亲代细胞中相应多萜基衍生物的水平进行了比较。尽管合成速率降低,但通过以较低速率利用这些中间体,发现CHB11 - 1 - 3能维持接近正常水平的Man5GlcNAc2 - P - P - 聚戊烯醇和甘露糖基磷酸化聚戊烯醇。通过乙酰解确定,连接在CHB11 - 1 - 3细胞中聚戊烯醇和亲代细胞中多萜醇上的Man5GlcNAc2寡糖结构相同。在体外反应中,Man5GlcNAc2 - P - P - 聚戊烯醇和Man5GlcNAc5 - P - P - 多萜醇似乎都能有效转运。比较了水疱性口炎病毒(VSV)感染的亲代细胞和突变体细胞中G蛋白的糖基化情况;尽管在水疱性口炎病毒(VSV)感染的亲代细胞和突变体细胞中对一部分G蛋白进行了比较;尽管在CHB11 - 1 - 3细胞中有一部分G蛋白正常糖基化,但大部分G蛋白糖基化不足,导致G蛋白上要么添加一个寡糖,要么不添加寡糖。添加单个寡糖是随机发生的而非优先发生在两个位点之一。

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