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肝素裂解酶 I 催化肝素解聚的结构快照

Structural snapshots of heparin depolymerization by heparin lyase I.

作者信息

Han Young-Hyun, Garron Marie-Line, Kim Hye-Yeon, Kim Wan-Seok, Zhang Zhenqing, Ryu Kyeong-Seok, Shaya David, Xiao Zhongping, Cheong Chaejoon, Kim Yeong Shik, Linhardt Robert J, Jeon Young Ho, Cygler Miroslaw

机构信息

Magnetic Resonance Team, Korea Basic Science Institute, Ochang, Chungbuk 363-883, Korea.

出版信息

J Biol Chem. 2009 Dec 4;284(49):34019-27. doi: 10.1074/jbc.M109.025338. Epub 2009 Oct 2.

DOI:10.1074/jbc.M109.025338
PMID:19801541
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2797172/
Abstract

Heparin lyase I (heparinase I) specifically depolymerizes heparin, cleaving the glycosidic linkage next to iduronic acid. Here, we show the crystal structures of heparinase I from Bacteroides thetaiotaomicron at various stages of the reaction with heparin oligosaccharides before and just after cleavage and product disaccharide. The heparinase I structure is comprised of a beta-jellyroll domain harboring a long and deep substrate binding groove and an unusual thumb-resembling extension. This thumb, decorated with many basic residues, is of particular importance in activity especially on short heparin oligosaccharides. Unexpected structural similarity of the active site to that of heparinase II with an (alpha/alpha)(6) fold is observed. Mutational studies and kinetic analysis of this enzyme provide insights into the catalytic mechanism, the substrate recognition, and processivity.

摘要

肝素酶I(heparinase I)能特异性地使肝素解聚,切割艾杜糖醛酸旁边的糖苷键。在此,我们展示了来自嗜热栖热放线杆菌的肝素酶I在与肝素寡糖反应的不同阶段(切割前、切割后即刻以及产物二糖)的晶体结构。肝素酶I的结构由一个具有长而深的底物结合凹槽的β-果冻卷结构域和一个不寻常的类似拇指的延伸部分组成。这个拇指状结构带有许多碱性残基,在活性方面尤其对短肝素寡糖起着特别重要的作用。观察到该活性位点与具有(α/α)(6)折叠结构的肝素酶II的活性位点存在意想不到的结构相似性。对该酶的突变研究和动力学分析为催化机制、底物识别和持续性提供了深入见解。

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