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用于深入了解糖基化模式与生物活性之间关系的促红细胞生成素糖型的化学合成。

Chemical synthesis of erythropoietin glycoforms for insights into the relationship between glycosylation pattern and bioactivity.

作者信息

Murakami Masumi, Kiuchi Tatsuto, Nishihara Mika, Tezuka Katsunari, Okamoto Ryo, Izumi Masayuki, Kajihara Yasuhiro

机构信息

Department of Chemistry, Osaka University, 1-1, Machikaneyama, Toyonaka, Osaka 5460-0043, Japan.

Glytech Inc., 134, Chudoji, Minamimachi KRP#1-109, Shimogyo-ku, Kyoto 600-8813, Japan.

出版信息

Sci Adv. 2016 Jan 15;2(1):e1500678. doi: 10.1126/sciadv.1500678. eCollection 2016 Jan.

Abstract

The role of sialyloligosaccharides on the surface of secreted glycoproteins is still unclear because of the difficulty in the preparation of sialylglycoproteins in a homogeneous form. We selected erythropoietin (EPO) as a target molecule and designed an efficient synthetic strategy for the chemical synthesis of a homogeneous form of five EPO glycoforms varying in glycosylation position and the number of human-type biantennary sialyloligosaccharides. A segment coupling strategy performed by native chemical ligation using six peptide segments including glycopeptides yielded homogeneous EPO glycopeptides, and folding experiments of these glycopeptides afforded the correctly folded EPO glycoforms. In an in vivo erythropoiesis assay in mice, all of the EPO glycoforms displayed biological activity, in particular the EPO bearing three sialyloligosaccharides, which exhibited the highest activity. Furthermore, we observed that the hydrophilicity and biological activity of the EPO glycoforms varied depending on the glycosylation pattern. This knowledge will pave the way for the development of homogeneous biologics by chemical synthesis.

摘要

由于难以制备出均一形式的唾液酸化糖蛋白,分泌型糖蛋白表面唾液酸化低聚糖的作用仍不清楚。我们选择促红细胞生成素(EPO)作为目标分子,并设计了一种高效的合成策略,用于化学合成五种糖基化位置和人源型双天线唾液酸化低聚糖数量不同的均一形式的EPO糖型。通过使用包括糖肽在内的六个肽段进行天然化学连接的片段偶联策略,得到了均一的EPO糖肽,对这些糖肽进行折叠实验得到了正确折叠的EPO糖型。在小鼠体内的红细胞生成试验中,所有EPO糖型均表现出生物活性,尤其是带有三个唾液酸化低聚糖的EPO,其活性最高。此外,我们观察到EPO糖型的亲水性和生物活性因糖基化模式而异。这一知识将为通过化学合成开发均一生物制品铺平道路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5737/4730857/bd0de4a46b73/1500678-F1.jpg

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