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α3唾液酸化且多聚α3岩藻糖基化的双天线聚乳糖胺的酶促合成。一种二价[sialyl diLex] - 二糖可选择性地抑制淋巴细胞与内皮细胞的器官特异性黏附。

Enzymatic synthesis of alpha3'sialylated and multiply alpha3fucosylated biantennary polylactosamines. A bivalent [sialyl diLex]-saccharide inhibited lymphocyte-endothelium adhesion organ-selectively.

作者信息

Toppila S, Renkonen R, Penttilä L, Natunen J, Salminen H, Helin J, Maaheimo H, Renkonen O

机构信息

Haartman Institute, Department of Bacteriology and Immunology, Institute of Biotechnology, University of Helsinki, Finland.

出版信息

Eur J Biochem. 1999 Apr;261(1):208-15. doi: 10.1046/j.1432-1327.1999.00257.x.

DOI:10.1046/j.1432-1327.1999.00257.x
PMID:10103052
Abstract

Multifucosylated sialo-polylactosamines are known to be high affinity ligands for E-selectin. PSGL-1, the physiological ligand of P-selectin, is decorated in HL-60 cells by a sialylated and triply fucosylated polylactosamine that is believed to be of functional importance. Mimicking some of these saccharide structures, we have synthesized enzymatically a bivalent [sialyl diLex]-glycan, Neu5Acalpha2-3'Lexbeta1-3'Lexbeta1-3'(Neu5Acalpha2-3'Lexbeta1-3Lexbe ta1-6')LN [where Neu5Ac is N-acetylneuraminic acid, Lex is the trisaccharide Galbeta1-4(Fucalpha1-3)GlcNAc and LN is the disaccharide Galbeta1-4GlcNAc]. Several structurally related, novel polylactosamine glycans were also constructed. The inhibitory effects of these glycans on two L-selectin-dependent, lymphocyte-to-endothelium adhesion processes of rats were analysed in ex-vivo Stamper-Woodruff binding assays. The IC50 value of the bivalent [sialyl diLex]-glycan at lymph node high endothelium was 50 nm, but at the capillaries of rejecting cardiac allografts it was only 5 nm. At both adhesion sites, the inhibition was completely dependent on the presence of fucose units on the sialylated LN units of the inhibitor saccharide. These data show that the bivalent [sialyl diLex]-glycan is a high affinity ligand for L-selectin, and may reduce extravasation of lymphocytes at sites of inflammation in vivo without severely endangering the normal recirculation of lymphocytes via lymph nodes.

摘要

多岩藻糖基化唾液酸 - 聚乳糖胺是已知的E - 选择素的高亲和力配体。PSGL - 1是P - 选择素的生理配体,在HL - 60细胞中被一种唾液酸化且三重岩藻糖基化的聚乳糖胺修饰,据信这种修饰具有功能重要性。模仿其中一些糖结构,我们通过酶法合成了一种二价的[sialyl diLex] - 聚糖,即Neu5Acalpha2 - 3'Lexbeta1 - 3'Lexbeta1 - 3'(Neu5Acalpha2 - 3'Lexbeta1 - 3Lexbeta1 - 6')LN [其中Neu5Ac是N - 乙酰神经氨酸,Lex是三糖Galbeta1 - 4(Fucalpha1 - 3)GlcNAc,LN是二糖Galbeta1 - 4GlcNAc]。还构建了几种结构相关的新型聚乳糖胺聚糖。在体外Stamper - Woodruff结合试验中分析了这些聚糖对大鼠两种L - 选择素依赖性淋巴细胞与内皮细胞粘附过程的抑制作用。二价[sialyl diLex] - 聚糖在淋巴结高内皮处的IC50值为50 nM,但在排斥心脏同种异体移植的毛细血管处仅为5 nM。在两个粘附位点,抑制作用完全取决于抑制剂糖的唾液酸化LN单元上岩藻糖单元的存在。这些数据表明,二价[sialyl diLex] - 聚糖是L - 选择素的高亲和力配体,并且在体内炎症部位可能减少淋巴细胞的外渗,而不会严重危及淋巴细胞通过淋巴结的正常再循环。

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