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三种不同糖基化形式的重组人粒细胞巨噬细胞集落刺激因子的纯化与特性分析

Purification and characterization of three forms of differently glycosylated recombinant human granulocyte-macrophage colony-stimulating factor.

作者信息

Okamoto M, Nakai M, Nakayama C, Yanagi H, Matsui H, Noguchi H, Namiki M, Sakai J, Kadota K, Fukui M

机构信息

Takarazuka Research Center, Sumitomo Chemical Co., Ltd., Hyogo, Japan.

出版信息

Arch Biochem Biophys. 1991 May 1;286(2):562-8. doi: 10.1016/0003-9861(91)90080-3.

DOI:10.1016/0003-9861(91)90080-3
PMID:1897978
Abstract

We have purified recombinant human granulocyte-macrophage colony-stimulating factor (hGM-CSF) produced in human lymphoblastoid Namalwa cells. From the results of tunicamycin treatment and N-glycosidase F digestion, it was demonstrated that Namalwa-derived hGM-CSF was highly glycosylated at two potential N-glycosylation sites and several O-glycosylation sites as previously shown for naturally occurring hGM-CSF. We classified the hGM-CSF molecules into three groups according to the molecular weight corresponding to the degree of N-glycosylation: the molecules with two N-glycosylation sites occupied (designated 2N), the molecules with either site glycosylated (1N), and the molecules lacking N-glycosylation (0N). Despite such varied degrees of N-glycosylation, almost all molecules were O-glycosylated. To investigate the role of carbohydrate moieties of hGM-CSF, we isolated each form of hGM-CSF and examined its biological properties. The 2N-type showed 200-fold less in vitro specific activity compared with unglycosylated Escherichia coli-derived hGM-CSF, although the activity of the 0N-type was equivalent to that of the E. coli-derived material. The 1N-type showed an intermediate level of activity. However, in terms of clearance from blood circulation in the rat, the 2N-type showed a half-life five times longer than that of the 0N-type and E. coli-derived hGM-CSF. From these findings, we concluded that N-linked carbohydrate moieties of hGM-CSF play conflicting physiological roles in the efficacy of the protein in vivo but that O-linked carbohydrate moieties do not have such effects.

摘要

我们已经纯化了在人淋巴母细胞Namalwa细胞中产生的重组人粒细胞-巨噬细胞集落刺激因子(hGM-CSF)。从衣霉素处理和N-糖苷酶F消化的结果表明,如先前对天然存在的hGM-CSF所示,Namalwa来源的hGM-CSF在两个潜在的N-糖基化位点和几个O-糖基化位点高度糖基化。我们根据与N-糖基化程度相对应的分子量将hGM-CSF分子分为三组:两个N-糖基化位点均被占据的分子(称为2N)、其中一个位点被糖基化的分子(1N)和缺乏N-糖基化的分子(0N)。尽管N-糖基化程度不同,但几乎所有分子都进行了O-糖基化。为了研究hGM-CSF碳水化合物部分的作用,我们分离了每种形式的hGM-CSF并检测其生物学特性。2N型与未糖基化的大肠杆菌来源的hGM-CSF相比,体外比活性低200倍,尽管0N型的活性与大肠杆菌来源的材料相当。1N型表现出中等水平的活性。然而,就大鼠血液循环中的清除率而言,2N型的半衰期比0N型和大肠杆菌来源的hGM-CSF长五倍。从这些发现中我们得出结论,hGM-CSF的N-连接碳水化合物部分在该蛋白体内功效方面发挥着相互矛盾的生理作用,但O-连接碳水化合物部分没有这种作用。

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