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Biosynthesis of Natural and Hyperelongated Chondroitin Sulfate Glycosaminoglycans: New Insights into an Elusive Process

机译:天然和超长硫酸软骨素糖胺聚糖的生物合成:难以捉摸的过程的新见解。

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摘要

Proteoglycans are important components of the extracellular matrix of all tissues. Proteoglycans are comprised of a core protein and one or more covalently attached glycosaminoglycan (GAG) chains. The major chondroitin sulfate (CS) and dermatan sulfate (DS) proteoglycans are aggrecan, versican, biglycan and decorin. Cells synthesize GAGs of natural or basal lengths and the GAG chains are subject to considerable growth factor, hormonal and metabolic regulation to yield longer GAG chains with altered structure and function. The mechanism by which the CS/DS GAG chains are polymerized is unknown. Recent work has identified several monosaccharide transferases which when co-expressed yield GAG polymers and the length of the polymers depends upon the pair of enzymes coexpressed. The further extension of these chains is regulated by signaling pathways. Inhibition of these latter pathways may be a therapeutic target to prevent the elongation which is associated with increased binding of atherogenic lipids and the disease process of atherosclerosis.
机译:蛋白聚糖是所有组织细胞外基质的重要组成部分。蛋白聚糖由核心蛋白和一个或多个共价连接的糖胺聚糖(GAG)链组成。硫酸软骨素(CS)和硫酸皮肤素(DS)的主要蛋白聚糖是聚集蛋白聚糖,versican,biglycan和decorin。细胞合成天然或基础长度的GAG,GAG链受到相当大的生长因子,激素和代谢调节,以产生结构和功能改变的更长GAG链。 CS / DS GAG链聚合的机理尚不清楚。最近的工作已经鉴定了几种单糖转移酶,当它们共表达时会产生GAG聚合物,并且聚合物的长度取决于共表达的酶对。这些链的进一步延伸由信号传导途径调控。抑制这些后面的途径可能是预防延长的治疗靶点,所述延长与动脉粥样硬化脂质的结合增加和动脉粥样硬化的疾病过程有关。

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