首页> 外文期刊>Virchows Archiv >Cartilage tumour progression is characterized by an increased expression of heparan sulphate 6O-sulphation-modifying enzymes
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Cartilage tumour progression is characterized by an increased expression of heparan sulphate 6O-sulphation-modifying enzymes

机译:软骨肿瘤进展的特征是硫酸乙酰肝素6O硫酸化修饰酶的表达增加

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Chondrosarcomas are malignant cartilage-forming tumours that can arise centrally (in the medulla) or peripherally (at the surface) of the bone. They are classified into three histological grades which correspond to the clinical severity. Previous studies by our group have shown altered signal transduction of the fibroblast growth factor and Wnt signalling pathways during peripheral chondrosarcoma progression. Heparan sulphate (HS) is a glycosaminoglycan that facilitates receptor binding of multiple growth factors, in which the sulphation of 6O position plays a pivotal role. 6O-Sulphation occurs through three HS 6O-sulphotransferases (HS6ST1-3) and is fine-tuned by two endosulphatases (SULF1-2) that remove 6O-sulphate groups. We have investigated whether the expression of HS6STs and SULFs changes during chondrosarcoma progression and have determined 6O-sulphation levels in two chondrosarcoma cell lines. Immunohistochemistry on tissue microarrays of chondrosarcomas showed that HS6ST3 and SULF1 were highly expressed in most chondrosarcomas, whereas SULF2 expression was absent in most cases. HS6ST1 and HS6ST2 expression are significantly increased during chondrosarcoma progression, which suggest that 6O-sulphation is increased during progression. This was confirmed in one grade III chondrosarcoma cell line, which showed a dramatically increased 6O-sulphation compared to an articular chondrocyte cell line by HPLC; another cell line showed an increased expression of one 6O-sulphated HS disaccharide. In conclusion, our results show increased HS6ST1 and HS6ST2 expression during chondrosarcoma progression and increased HS 6O-sulphation in vitro. As 6O-sulphation plays an important role in signal transduction, altered HS6ST expression might be associated with changes in signal transduction pathways in chondrosarcoma progression.
机译:软骨肉瘤是形成软骨的恶性肿瘤,可在骨的中央(在延髓中)或外周(在表面处)出现。它们分为与临床严重程度相对应的三个组织学等级。我们小组先前的研究表明,在周围软骨肉瘤进展过程中,成纤维细胞生长因子和Wnt信号通路的信号转导发生了改变。硫酸乙酰肝素(HS)是一种糖胺聚糖,可促进多种生长因子的受体结合,其中6O位置的硫酸化起关键作用。 6O-硫酸化通过三个HS 6O-硫酸转移酶(HS6ST1-3)发生,并且通过去除6O-硫酸盐基团的两个内硫酸盐酶(SULF1-2)进行微调。我们调查了软骨肉瘤进展过程中HS6STs和SULFs的表达是否发生变化,并确定了两种软骨肉瘤细胞系中的6O硫酸化水平。软骨肉瘤组织芯片上的免疫组织化学显示,HS6ST3和SULF1在大多数软骨肉瘤中高表达,而在大多数情况下SULF2表达不存在。 HS6ST1和HS6ST2的表达在软骨肉瘤发展过程中显着增加,这表明在发展过程中6O硫酸化增加。这在一种III级软骨肉瘤细胞系中得到了证实,与HPLC的关节软骨细胞系相比,它显示出6O硫酸盐的急剧增加。另一细胞系显示一种6O硫酸化的HS二糖的表达增加。总之,我们的结果显示,软骨肉瘤进展期间HS6ST1和HS6ST2表达增加,体外HS 6O硫酸化增加。由于6O硫化在信号转导中起重要作用,因此改变的HS6ST表达可能与软骨肉瘤进展中信号转导途径的改变有关。

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