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Structure-based engineering of heparinase I with improved specific activity for degrading heparin

机译：具有改进的比活性的肝素酶I的基于结构的工程设计可降解肝素

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摘要

BackgroundHeparinase I from Pedobacter heparinus (Ph-HepI), which specifically cleaves heparin and heparan sulfate, is one of the most extensively studied glycosaminoglycan lyases. Enzymatic degradation of heparin by heparin lyases not only largely facilitates heparin structural analysis but also showed great potential to produce low-molecular-weight heparin (LMWH) in an environmentally friendly way. However, industrial applications of Ph-HepI have been limited by their poor yield and enzyme activity. In this work, we improve the specific enzyme activity of Ph-HepI based on homology modeling, multiple sequence alignment, molecular docking and site-directed mutagenesis.

机译：背景技术肝Pedobacter heparinus（Ph-HepI）的肝素酶I是特异地裂解肝素和硫酸乙酰肝素的酶，是研究最广泛的糖胺聚糖裂解酶之一。肝素裂解酶对肝素的酶降解作用不仅在很大程度上促进了肝素的结构分析，而且还显示出以环保的方式生产低分子量肝素（LMWH）的巨大潜力。但是，Ph-HepI的工业应用受到产量和酶活性差的限制。在这项工作中，我们基于同源性建模，多序列比对，分子对接和定点诱变提高了Ph-HepI的比酶活性。

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期刊名称 BMC Biotechnology
作者
Chuan Zhang; Bao-Cheng Yang; Wen-Ting Liu; Zhong-Yuan Li; Ya-Jian Song; Tong-Cun Zhang; Xue-Gang Luo;
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作者单位

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年(卷),期 2019(19),-1
年度 2019
页码 59
总页数 12
原文格式 PDF
正文语种
中图分类应用微生物学;
关键词
Heparinase I Specific activity Site-directed mutagenesis Homology modeling Molecular docking;

机译：肝素酶I;比活;定点诱变;同源性建模;分子对接;

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专利

1. Improving the activity of heparinase I by the directed evolution, its enzymatic properties and optimal conditions for heparin degrading by recombinant cells [J] . Yu Ping, Jia Tianmei, Chen Yanxia, Biochemical Engineering Journal . 2016,第Null期

机译：通过定向进化，其酶学性质和重组细胞降解肝素的最佳条件来改善肝素酶I的活性
2. Heparinase I-specific disaccharide unit of heparin is a key structure but insufficient for exerting anti-prion activity in prion-infected cells [J] . Teruya Kenta, Wakao Masahiro, Sato Masaki, Biochemical and Biophysical Research Communications . 2015,第4期

机译：肝素的肝素酶I特异性二糖单元是关键结构，但不足以在感染ion病毒的细胞中发挥抗-病毒活性
3. Improving the specific activity of β-mannanase from Aspergillus niger BK01 by structure-based rational design [J] . HuangJ.-W., ChenC.-C., HuangC.-H., Biochimica et biophysica acta: BBA: International journal of biochemistry, biophysics and molecular biololgy. Proteins and Proteomics . 2014,第3期

机译：通过基于结构的合理设计提高黑曲霉BK01中β-甘露聚糖酶的比活性
4. Substrate specificity of heparinase from a species of Sphingobacter -ium sp [C] . Chao Yapeng, Qian Shijun, Cheng Xiulan The Seventh China-Japan joint symposium on enzyme engineering . 2002

机译：某种Sphingobacter -ium sp肝素酶的底物特异性
5. Improved heparin therapeutics: Biocompatible composites & redesigning the biological activities of heparin on microarray chips. [D] . Park, Tae-Joon. 2008

机译：改进的肝素疗法：生物相容性复合材料，并重新设计肝素在微阵列芯片上的生物活性。
6. Engineering of CYP76AH15 can improve activity and specificity towards forskolin biosynthesis in yeast [O] . Victor Forman, Niels Bjerg-Jensen, Jane D. Dyekjær, 2018

机译：CYP76AH15的工程改造可提高酵母中毛喉素生物合成的活性和特异性
7. Structure-based engineering of heparinase I with improved specific activity for degrading heparin [O] . Chuan Zhang, Bao-Cheng Yang, Wen-Ting Liu, 2019

机译：肝素酶I基于结构的工程，改善了降解肝素的特异性活性

Structure-based engineering of heparinase I with improved specific activity for degrading heparin

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