首页> 外文OA文献 >A family of novel, acidic N-glycans in Bowes melanoma tissue plasminogen activator have L2/HNK-1-bearing antennae, many with sulfation of the fucosylated chitobiose core.
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A family of novel, acidic N-glycans in Bowes melanoma tissue plasminogen activator have L2/HNK-1-bearing antennae, many with sulfation of the fucosylated chitobiose core.

机译:Bowes黑色素瘤组织纤溶酶原激活物中的一类新型酸性N-聚糖具有L2 / HNK-1的触角,其中许多具有岩藻糖基化的壳二糖核心被硫酸化。

摘要

A family of about 20 novel acidic bi- and tri-antennary N-glycans, amounting to almost half those expressed on Bowes melanoma tissue-plasminogen activator (t-PA) were found to possess Galbeta1-->4GlcNAcbeta1-->, sulfated and sialylated GalNAcbeta1-->4GlcNAcbeta1--> or sulfated GlcAbeta1--> 3Galbeta1-->4GlcNAcbeta1--> antennae, of which those containing sulfated GlcA, depicting the L2/HNK-1 carbohydrate epitope, were preferentially located on the 6 arm. A proportion of the glycans were highly charged, because of multiple and variously distributed sulfation, some of which was located on the fucosylated chitobiose core. Multiple expression of the L2/HNK-1 epitope on a single glycan was observed. The most abundant compound was a biantennary glycan carrying sulfated GlcA on the 6-branched antenna and an alpha2-->6 sialylated GalNAc on the other. The N-glycosylation sequon containing Asn448, which is known to express all of the sulfate-carrying N-glycans contains, unusually, an arginine residue. An electrostatic interaction between this cationic amino acid and the core-sulfate group of the N-glycan is proposed to reduce mobility of the carbohydrate in the region of the t-PA active site. Because of the 'brain-type' nature of the N-glycans described in this neuro-ectodermal cell line, the possibility of neural t-PA interacting with the L2/HNK-1-recognizing molecule, laminin, of the central nervous system extracellular matrix is discussed.
机译:发现大约20个新的酸性双和三触角N-聚糖家族,几乎占Bowes黑色素瘤组织纤溶酶原激活剂(t-PA)上表达的一半,具有Galbeta1-> 4GlcNAcbeta1->,被硫酸化和唾液酸化的GalNAcbeta1→4GlcNAcbeta1→或硫酸化的GlcAbeta1→3Galbeta1→4GlcNAcbeta1→触角,其中含有硫酸化GlcA的L2 / HNK-1碳水化合物表位的触角优先位于6臂上。由于多种和多种分布的硫酸化作用,一部分聚糖带高电荷,其中一些位于岩藻糖基化的壳二糖核心上。观察到在单个聚糖上L2 / HNK-1表位的多种表达。最丰富的化合物是在6分支触角上带有硫酸化GlcA的双触角聚糖,在另一个上带有α2-> 6唾液酸化的GalNAc。含有Asn448的N-糖基化序列(已知能表达所有带有硫酸盐的N-聚糖)通常含有精氨酸残基。该阳离子氨基酸和N-聚糖的核心硫酸根基团之间的静电相互作用被提出来减少碳水化合物在t-PA活性位点区域中的迁移率。由于此神经外胚层细胞系中描述的N聚糖具有“大脑型”性质,因此神经t-PA与细胞外中枢神经系统的L2 / HNK-1识别分子层粘连蛋白相互作用的可能性讨论矩阵。

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