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2
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Two distinct alpha-L-fucosidases from Bifidobacterium bifidum are essential for the utilization of fucosylated milk oligosaccharides and glycoconjugates.来自两歧双歧杆菌的两种不同的α-L-岩藻糖苷酶对于利用岩藻糖基化乳寡糖和糖缀合物至关重要。
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A remodeling system of the 3'-sulfo-Lewis a and 3'-sulfo-Lewis x epitopes.3'-磺基路易斯a和3'-磺基路易斯x表位的重塑系统
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7
The ruminant parasite Haemonchus contortus expresses an alpha1,3-fucosyltransferase capable of synthesizing the Lewis x and sialyl Lewis x antigens.反刍动物寄生虫捻转血矛线虫表达一种能够合成Lewis x和唾液酸化Lewis x抗原的α1,3-岩藻糖基转移酶。
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Immobilized Lotus tetragonolobus agglutinin binds oligosaccharides containing the Le(x) determinant.固定化的百脉根凝集素可结合含有Le(x)决定簇的寡糖。
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Processing of X-ray diffraction data collected in oscillation mode.振荡模式下收集的X射线衍射数据的处理。
Methods Enzymol. 1997;276:307-26. doi: 10.1016/S0076-6879(97)76066-X.
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Bifidobacterium longum subsp. infantis ATCC 15697 α-fucosidases are active on fucosylated human milk oligosaccharides.长双歧杆菌亚种。婴儿 ATCC 15697 α-岩藻糖苷酶在岩藻糖基化的人乳低聚糖上具有活性。
Appl Environ Microbiol. 2012 Feb;78(3):795-803. doi: 10.1128/AEM.06762-11. Epub 2011 Dec 2.
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Bifidobacterium longum subsp. infantis uses two different β-galactosidases for selectively degrading type-1 and type-2 human milk oligosaccharides.长双歧杆菌亚种。婴儿使用两种不同的β-半乳糖苷酶有选择地降解 1 型和 2 型人乳寡糖。
Glycobiology. 2012 Mar;22(3):361-8. doi: 10.1093/glycob/cwr116. Epub 2011 Sep 16.
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Physiology of consumption of human milk oligosaccharides by infant gut-associated bifidobacteria.人乳寡糖被婴儿肠道相关双歧杆菌消耗的生理学。
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Utilization of natural fucosylated oligosaccharides by three novel alpha-L-fucosidases from a probiotic Lactobacillus casei strain.新型益生菌干酪乳杆菌来源的α-L-岩藻糖苷酶对天然岩藻糖基化低聚糖的利用
Appl Environ Microbiol. 2011 Jan;77(2):703-5. doi: 10.1128/AEM.01906-10. Epub 2010 Nov 19.
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A novel alpha-D-galactosynthase from Thermotoga maritima converts beta-D-galactopyranosyl azide to alpha-galacto-oligosaccharides.一种新型的来自海洋栖热菌的α-D-半乳糖合酶将β-D-半乳糖基叠氮化物转化为α-半乳糖低聚糖。
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Features and development of Coot.Coot的特点与发展
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Structural basis of alpha-fucosidase inhibition by iminocyclitols with K(i) values in the micro- to picomolar range.抑制常数(Ki)值在微摩尔至皮摩尔范围内的亚氨基环醇对α-岩藻糖苷酶的抑制作用的结构基础。
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beta-Glycosyl azides as substrates for alpha-glycosynthases: preparation of efficient alpha-L-fucosynthases.β-糖基叠氮化物作为α-糖苷合成酶的底物:高效α-L-岩藻糖合成酶的制备
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One-pot enzymatic production of beta-D-galactopyranosyl-(1-->3)-2-acetamido-2-deoxy-D-galactose (galacto-N-biose) from sucrose and 2-acetamido-2-deoxy-D-galactose (N-acetylgalactosamine).一锅法酶法合成蔗糖和 2-乙酰氨基-2-脱氧-D-半乳糖(N-乙酰氨基半乳糖)生成β-D-半乳糖基-(1-->3)-2-乙酰氨基-2-脱氧-D-半乳糖(半乳糖-N-双糖)。
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特异性地将 Lewis a/x 抗原引入到类型 1/2 链中的 1,3-1,4-α-L-岩藻糖基转移酶。

1,3-1,4-α-L-fucosynthase that specifically introduces Lewis a/x antigens into type-1/2 chains.

机构信息

Research Institute for Bioresources and Biotechnology, Ishikawa Prefectural University, Nonoichi, Ishikawa 921-8836, Japan.

出版信息

J Biol Chem. 2012 May 11;287(20):16709-19. doi: 10.1074/jbc.M111.333781. Epub 2012 Mar 26.

DOI:10.1074/jbc.M111.333781
PMID:22451675
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3351332/
Abstract

α-L-fucosyl residues attached at the non-reducing ends of glycoconjugates constitute histo-blood group antigens Lewis (Le) and ABO and play fundamental roles in various biological processes. Therefore, establishing a method for synthesizing the antigens is important for functional glycomics studies. However, regiospecific synthesis of glycosyl linkages, especially α-L-fucosyl linkages, is quite difficult to control both by chemists and enzymologists. Here, we generated an α-L-fucosynthase that specifically introduces Le(a) and Le(x) antigens into the type-1 and type-2 chains, respectively; i.e. the enzyme specifically accepts the disaccharide structures (Galβ1-3/4GlcNAc) at the non-reducing ends and attaches a Fuc residue via an α-(1,4/3)-linkage to the GlcNAc. X-ray crystallographic studies revealed the structural basis of this strict regio- and acceptor specificity, which includes the induced fit movement of the catalytically important residues, and the difference between the active site structures of 1,3-1,4-α-L-fucosidase (EC 3.2.1.111) and α-L-fucosidase (EC 3.2.1.51) in glycoside hydrolase family 29. The glycosynthase developed in this study should serve as a potentially powerful tool to specifically introduce the Le(a/x) epitopes onto labile glycoconjugates including glycoproteins. Mining glycosidases with strict specificity may represent the most efficient route to the specific synthesis of glycosidic bonds.

摘要

α-L-岩藻糖残基连接在糖缀合物的非还原末端构成了组织血型抗原 Lewis(Le)和 ABO,并在各种生物过程中发挥着重要作用。因此,建立合成这些抗原的方法对于功能糖组学研究非常重要。然而,糖苷键的区域特异性合成,特别是α-L-岩藻糖键的合成,无论是化学家还是酶学家都很难控制。在这里,我们生成了一种α-L-岩藻糖合酶,它可以分别将 Le(a)和 Le(x)抗原引入到 1 型和 2 型链中;即,该酶特异性地接受非还原末端的二糖结构(Galβ1-3/4GlcNAc),并通过α-(1,4/3)-键将岩藻糖残基连接到 GlcNAc 上。X 射线晶体学研究揭示了这种严格的区域和受体特异性的结构基础,包括催化重要残基的诱导契合运动,以及糖苷水解酶家族 29 中 1,3-1,4-α-L-岩藻糖苷酶(EC 3.2.1.111)和α-L-岩藻糖苷酶(EC 3.2.1.51)的活性位点结构之间的差异。本研究开发的糖基合成酶应该成为一种潜在的强大工具,可以将 Le(a/x)表位特异性地引入包括糖蛋白在内的不稳定糖缀合物上。挖掘具有严格特异性的糖苷酶可能代表了特定合成糖苷键的最有效途径。