Xanthine oxidase inhibitory peptides derived from tuna protein: virtual screening, inhibitory activity, and molecular mechanisms

被引:33
|
作者
Yu, Zhipeng [1 ]
Kan, Ruotong [1 ]
Wu, Sijia [1 ]
Guo, Hui [1 ]
Zhao, Wenzhu [1 ]
Ding, Long [2 ]
Zheng, Fuping [3 ]
Liu, Jingbo [4 ]
机构
[1] Bohai Univ, Coll Food Sci & Engn, Jinzhou City 121013, Liaoning, Peoples R China
[2] Northwest A&F Univ, Coll Food Sci & Engn, Yangling, Shaanxi, Peoples R China
[3] Beijing Technol & Business Univ BTBU, Beijing Adv Innovat Ctr Food Nutr & Human Hlth, Beijing, Peoples R China
[4] Jilin Univ, Lab Nutr & Funct Food, Changchun, Peoples R China
关键词
xanthine oxidase; inhibition mechanism; peptides; molecular docking; IN-VIVO; DARK MUSCLE; HYDROLYSATE; IDENTIFICATION; GOUT;
D O I
10.1002/jsfa.10745
中图分类号
S [农业科学];
学科分类号
09 ;
摘要
BACKGROUND There has been growing interest in the use of xanthine oxidase (XO) as a therapeutic agent to prevent gout and hyperuricemia. In the present study, XO inhibitory peptides were identified from tuna protein by virtual screening, and molecular docking was used to elicit the interaction mechanism between XO and peptides. RESULTS A novel tetrapeptide, EEAK, exhibited high XO inhibitory activity with an IC(50)of 173.00 +/- 0.06 mu M. Molecular docking analysis revealed that EEAK bound with the pivotal residues of XO's active sites (i.e., Glu802, Arg880, Glu1261) through two conventional hydrogen bond interactions, two attractive charge interactions, and one salt bridge. EEAK could also bind with the residues Phe649, Leu648, Lys771, Ser876, Phe914, and Thr1010 of XO. CONCLUSION This study suggested that conventional hydrogen bond interactions and electrostatic interactions play an important role in XO inhibition. The novel XO inhibitory peptide EEAK from tuna protein could be used as potential candidate for controlling gout and hyperuricemia. (c) 2020 Society of Chemical Industry
引用
收藏
页码:1349 / 1354
页数:6
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