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硫酸乙酰肝素生物合成酶EXT1和EXT2影响NDST1表达及硫酸乙酰肝素硫酸化。

Heparan sulfate biosynthesis enzymes EXT1 and EXT2 affect NDST1 expression and heparan sulfate sulfation.

作者信息

Presto Jenny, Thuveson Maria, Carlsson Pernilla, Busse Marta, Wilén Maria, Eriksson Inger, Kusche-Gullberg Marion, Kjellén Lena

机构信息

Department of Medical Biochemistry and Microbiology, Biomedical Center, University of Uppsala, Box 582, SE-751 23 Uppsala, Sweden.

出版信息

Proc Natl Acad Sci U S A. 2008 Mar 25;105(12):4751-6. doi: 10.1073/pnas.0705807105. Epub 2008 Mar 12.

Abstract

Heparan sulfate (HS) proteoglycans influence embryonic development and adult physiology through interactions with protein ligands. The interactions depend on HS structure, which is determined largely during biosynthesis by Golgi enzymes. How biosynthesis is regulated is more or less unknown. During polymerization of the HS chain, carried out by a complex of the exostosin proteins EXT1 and EXT2, the first modification enzyme, glucosaminyl N-deacetylase/N-sulfotransferase (NDST), introduces N-sulfate groups into the growing polymer. Unexpectedly, we found that the level of expression of EXT1 and EXT2 affected the amount of NDST1 present in the cell, which, in turn, greatly influenced HS structure. Whereas overexpression of EXT2 in HEK 293 cells enhanced NDST1 expression, increased NDST1 N-glycosylation, and resulted in elevated HS sulfation, overexpression of EXT1 had opposite effects. Accordingly, heart tissue from transgenic mice overexpressing EXT2 showed increased NDST activity. Immunoprecipitaion experiments suggested an interaction between EXT2 and NDST1. We speculate that NDST1 competes with EXT1 for binding to EXT2. Increased NDST activity in fibroblasts with a gene trap mutation in EXT1 supports this notion. These results support a model in which the enzymes of HS biosynthesis form a complex, or a GAGosome.

摘要

硫酸乙酰肝素(HS)蛋白聚糖通过与蛋白质配体相互作用影响胚胎发育和成年生理功能。这些相互作用取决于HS的结构,而HS结构在很大程度上是在生物合成过程中由高尔基体酶决定的。生物合成是如何被调控的,目前或多或少还不清楚。在由外切糖苷酶蛋白EXT1和EXT2组成的复合物进行HS链聚合过程中,第一种修饰酶,N-乙酰葡糖胺脱乙酰酶/N-硫酸转移酶(NDST),将N-硫酸基团引入正在生长的聚合物中。出乎意料的是,我们发现EXT1和EXT2的表达水平影响细胞中NDST1的含量,而这又极大地影响了HS的结构。在HEK 293细胞中过表达EXT2会增强NDST1表达,增加NDST1的N-糖基化,并导致HS硫酸化升高,而过表达EXT1则产生相反的效果。因此,过表达EXT2的转基因小鼠的心脏组织显示NDST活性增加。免疫沉淀实验表明EXT2与NDST1之间存在相互作用。我们推测NDST1与EXT1竞争与EXT2的结合。EXT1基因陷阱突变的成纤维细胞中NDST活性增加支持了这一观点。这些结果支持了一个模型,即HS生物合成的酶形成一个复合物,或称为糖胺聚糖体。

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