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来自福氏海参体壁的岩藻糖基化硫酸软骨素:构象、选择素结合及生物活性。

Fucosylated chondroitin sulfates from the body wall of the sea cucumber Holothuria forskali: conformation, selectin binding, and biological activity.

作者信息

Panagos Charalampos G, Thomson Derek S, Moss Claire, Hughes Adam D, Kelly Maeve S, Liu Yan, Chai Wengang, Venkatasamy Radhakrishnan, Spina Domenico, Page Clive P, Hogwood John, Woods Robert J, Mulloy Barbara, Bavington Charlie D, Uhrín Dušan

机构信息

From the EaStCHEM School of Chemistry, Joseph Black Building, The King's Buildings, University of Edinburgh, Edinburgh EH9 3JJ, United Kingdom.

GlycoMar Ltd., European Centre for Marine Biotechnology, Dunstaffnage Marine Laboratory, Oban, Argyll PA37 1QA, United Kingdom.

出版信息

J Biol Chem. 2014 Oct 10;289(41):28284-98. doi: 10.1074/jbc.M114.572297. Epub 2014 Aug 21.

DOI:10.1074/jbc.M114.572297
PMID:25147180
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4192483/
Abstract

Fucosylated chondroitin sulfate (fCS) extracted from the sea cucumber Holothuria forskali is composed of the following repeating trisaccharide unit: → 3)GalNAcβ4,6S(1 → 4) [FucαX(1 → 3)]GlcAβ(1 →, where X stands for different sulfation patterns of fucose (X = 3,4S (46%), 2,4S (39%), and 4S (15%)). As revealed by NMR and molecular dynamics simulations, the fCS repeating unit adopts a conformation similar to that of the Le(x) blood group determinant, bringing several sulfate groups into close proximity and creating large negative patches distributed along the helical skeleton of the CS backbone. This may explain the high affinity of fCS oligosaccharides for L- and P-selectins as determined by microarray binding of fCS oligosaccharides prepared by Cu(2+)-catalyzed Fenton-type and photochemical depolymerization. No binding to E-selectin was observed. fCS poly- and oligosaccharides display low cytotoxicity in vitro, inhibit human neutrophil elastase activity, and inhibit the migration of neutrophils through an endothelial cell layer in vitro. Although the polysaccharide showed some anti-coagulant activity, small oligosaccharide fCS fragments had much reduced anticoagulant properties, with activity mainly via heparin cofactor II. The fCS polysaccharides showed prekallikrein activation comparable with dextran sulfate, whereas the fCS oligosaccharides caused almost no effect. The H. forskali fCS oligosaccharides were also tested in a mouse peritoneal inflammation model, where they caused a reduction in neutrophil infiltration. Overall, the data presented support the action of fCS as an inhibitor of selectin interactions, which play vital roles in inflammation and metastasis progression. Future studies of fCS-selectin interaction using fCS fragments or their mimetics may open new avenues for therapeutic intervention.

摘要

从福氏海参(Holothuria forskali)中提取的岩藻糖基化硫酸软骨素(fCS)由以下重复三糖单元组成:→3)GalNAcβ4,6S(1→4)[FucαX(1→3)]GlcAβ(1→,其中X代表岩藻糖的不同硫酸化模式(X = 3,4S(46%)、2,4S(39%)和4S(15%))。核磁共振(NMR)和分子动力学模拟显示,fCS重复单元采用与Le(x)血型决定簇相似的构象,使多个硫酸基团紧密相邻,并在硫酸软骨素(CS)主链的螺旋骨架上形成大的负电荷区域。这可能解释了通过铜(2+)催化的芬顿型和光化学解聚制备的fCS寡糖的微阵列结合所确定的fCS寡糖对L-和P-选择素的高亲和力。未观察到与E-选择素的结合。fCS多糖和寡糖在体外显示出低细胞毒性,抑制人中性粒细胞弹性蛋白酶活性,并在体外抑制中性粒细胞通过内皮细胞层的迁移。尽管该多糖表现出一定的抗凝血活性,但小的fCS寡糖片段的抗凝血特性大大降低,其活性主要通过肝素辅因子II发挥。fCS多糖显示出与硫酸葡聚糖相当的前激肽释放酶激活作用,而fCS寡糖几乎没有影响。福氏海参fCS寡糖也在小鼠腹膜炎症模型中进行了测试,在该模型中它们导致中性粒细胞浸润减少。总体而言,所呈现的数据支持fCS作为选择素相互作用抑制剂的作用,选择素相互作用在炎症和转移进展中起着至关重要的作用。未来使用fCS片段或其模拟物对fCS-选择素相互作用的研究可能会为治疗干预开辟新途径。

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