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首页> 外文期刊>ACS Omega >Saccharide Primers Comprising Xylosyl-Serine Primed Phosphorylated Oligosaccharides Act as Intermediates in Glycosaminoglycan Biosynthesis
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Saccharide Primers Comprising Xylosyl-Serine Primed Phosphorylated Oligosaccharides Act as Intermediates in Glycosaminoglycan Biosynthesis

机译:包含木糖基-丝氨酸引发的磷酸化寡糖的糖质引物充当糖胺聚糖生物合成的中间体

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β-Xylosides have been used as an artificial initiator of glycosaminoglycan (GAG) biosynthesis to investigate its mechanism and to obtain these oligosaccharides. In GAG biosynthesis, phosphorylation on the xylose residue is a crucial step. However, little attention has been paid to phosphorylated oligosaccharides obtained from β-xylosides. In a previous study, we demonstrated that a novel β-xyloside, N -lauryl-O -β-xyloyranosyl-serinamide (Xyl-Ser-C12), had excellent GAG-type oligosaccharide priming ability, whereas phosphorylated oligosaccharides were not found in the primed oligosaccharides. This study examines the potential of Xyl-Ser-C12 and three of its derivatives for use as a probe to investigate the GAG biosynthesis mechanism. Glycosylated products were obtained by incubation of the β-xylosides in normal human dermal fibroblast cells and compared by liquid chromatography–electrospray ionization-mass spectrometry. By the optimized method to detect phosphorylated products, Xyl-Ser-C12 was demonstrated to prime not only GAG-type oligosaccharides but also a variety of xylose-phosphorylated products. Among the synthesized β-xylosides, those consisting of xylosyl-serine primed large amounts of phosphorylated and GAG-type oligosaccharides, whereas the others primed sialyloligosaccharides mainly. The majority of the phosphorylated products were considered to be GAG intermediates, which are less observed in nature. To our best knowledge, this is the first report showing that the amino acid residues around the Xyl attachment position strongly affect the phosphorylation efficiency and GAG chain-priming ability of β-xylosides. This study leads to the possibility of the use of β-xyloside as a probe to observe the Xyl phosphorylation process during GAG biosynthesis and investigate comparative glycosaminoglycomics between different cells.
机译:β-木糖苷已被用作糖胺聚糖(GAG)生物合成的人工引发剂,以研究其机理并获得这些寡糖。在GAG生物合成中,木糖残基上的磷酸化是至关重要的一步。然而,很少有人关注从β-木糖苷获得的磷酸化寡糖。在先前的研究中,我们证明了新型的β-木糖苷,N-月桂基-O-β-木聚糖基-丝氨酸酰胺(Xyl-Ser-C12)具有出色的GAG型寡糖引发能力,而磷酸化在引发的寡糖中未发现寡糖。这项研究检查了Xyl-Ser-C12及其三种衍生物作为研究GAG生物合成机制的探针的潜力。糖基化产物是通过在正常人皮肤成纤维细胞中孵育β-木糖苷得到的,并通过液相色谱-电喷雾电离质谱法进行比较。通过检测磷酸化产物的优化方法,已证明Xyl-Ser-C12不仅可以引发GAG型寡糖,而且可以引发多种木糖磷酸化产物。在合成的β-木糖苷中,由木糖基-丝氨酸组成的那些引发大量的磷酸化和GAG型寡糖,而其他的则主要引发唾液酸寡糖。大多数磷酸化产物被认为是GAG中间体,其在自然界中很少被观察到。据我们所知,这是第一个报告,表明Xyl附着位置周围的氨基酸残基强烈影响β-木糖苷的磷酸化效率和GAG链引发能力。这项研究导致使用β-木糖苷作为探针观察GAG生物合成过程中的Xyl磷酸化过程并研究不同细胞之间比较的糖胺糖组学的可能性。

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