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不同生产体系来源的重组β-葡糖苷脑苷脂酶的糖基化和功能。

Glycosylation and functionality of recombinant β-glucocerebrosidase from various production systems.

机构信息

*Protalix Biotherapeutics, 2 Snunit Street, P. O. Box 455, Carmiel, 2161401, Israel.

出版信息

Biosci Rep. 2013 Sep 25;33(5):e00071. doi: 10.1042/BSR20130081.

Abstract

The glycosylation of recombinant β-glucocerebrosidase, and in particular the exposure of mannose residues, has been shown to be a key factor in the success of ERT (enzyme replacement therapy) for the treatment of GD (Gaucher disease). Macrophages, the target cells in GD, internalize β-glucocerebrosidase through MRs (mannose receptors). Three enzymes are commercially available for the treatment of GD by ERT. Taliglucerase alfa, imiglucerase and velaglucerase alfa are each produced in different cell systems and undergo various post-translational or post-production glycosylation modifications to expose their mannose residues. This is the first study in which the glycosylation profiles of the three enzymes are compared, using the same methodology and the effect on functionality and cellular uptake is evaluated. While the major differences in glycosylation profiles reside in the variation of terminal residues and mannose chain length, the enzymatic activity and stability are not affected by these differences. Furthermore, the cellular uptake and in-cell stability in rat and human macrophages are similar. Finally, in vivo studies to evaluate the uptake into target organs also show similar results for all three enzymes. These results indicate that the variations of glycosylation between the three regulatory-approved β-glucocerebrosidase enzymes have no effect on their function or distribution.

摘要

重组β-葡糖脑苷脂酶的糖基化,特别是甘露糖残基的暴露,已被证明是 ERT(酶替代疗法)治疗 GD(戈谢病)成功的关键因素。巨噬细胞是 GD 的靶细胞,通过 MRs(甘露糖受体)内化β-葡糖脑苷脂酶。有三种酶可用于 ERT 治疗 GD。Taliglucerase alfa、imiglucerase 和 velaglucerase alfa 分别在不同的细胞系统中产生,并经历各种翻译后或生产后糖基化修饰,以暴露其甘露糖残基。这是首次使用相同的方法比较这三种酶的糖基化谱,并评估其对功能和细胞摄取的影响。虽然糖基化谱的主要差异在于末端残基和甘露糖链长的变化,但酶活性和稳定性不受这些差异的影响。此外,在大鼠和人巨噬细胞中的细胞摄取和细胞内稳定性也相似。最后,评估进入靶器官摄取的体内研究也显示出所有三种酶的相似结果。这些结果表明,三种监管批准的β-葡糖脑苷脂酶之间的糖基化差异对其功能或分布没有影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7cea/3782720/f7691de400ea/bsr2013-0081i001.jpg

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