Screen, Design and Enzymatic Activity Determination of Artificial Microperoxidases

被引:0
|
作者
Jia Xu
Xiaoming Zhao
Ye Yuan
Yanhui Song
Jiaqi Wang
Chonghan Wang
Yujia Chen
Jianing Wang
Zhijun Yan
Shuwen Guan
Liping Wang
机构
[1] Jilin University,School of Life Sciences
[2] China-Japan Union Hospital of Jilin University,Scientific Research Center
来源
Chemical Research in Chinese Universities | 2018年 / 34卷
关键词
Microperoxidase-11; Deuterohemin; Artificial microperoxidase; Enzymatic activity;
D O I
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中图分类号
学科分类号
摘要
Peroxidase activity greatly impacts the maintenance of free radical homeostasis, and can prevent or treat diseases related to free radicals. Microperoxidase-11(MP-11) is created via hydrolysis of cytochrome c iron-porphyrin complexes. In these complexes, the heme iron is penta-coordinate with histidine and exhibits excellent antioxidant activity when decomposing hydrogen peroxide. In this study, we screened the Ph.D.-7 and Ph.D.-12 phage display peptide libraries and obtained ten small peptide ligands of deuterohemin(the vinyl groups of oxidized heme). Among these polypeptides, DhHP-7P1, 12P1, 12P2 and 12P6 have good enzymatic activity compared with MP-11, and exhibit activities up to 50% of MP-11. Based on the screened sequences, we designed a series of artificial microperoxidases and determined that a higher peroxidase activity could be achieved with an enzymatic active site containing a second site of histidine residue spaced between two arginine residues with an interval of two amino acids(Dh-XHRXXR).
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页码:934 / 938
页数:4
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